Your search keyword '"Carlos A. DiazGranados"' showing total 79 results

1. A phase 1b randomized study of the safety and immunological responses to vaccination with H4:IC31, H56:IC31, and BCG revaccination in Mycobacterium tuberculosis-uninfected adolescents in Cape Town, South Africa

Author

Linda-Gail Bekker, One Dintwe, Andrew Fiore-Gartland, Keren Middelkoop, Julia Hutter, Anthony Williams, April K. Randhawa, Morten Ruhwald, Ingrid Kromann, Peter L. Andersen, Carlos A. DiazGranados, Kathryn T. Rutkowski, Dereck Tait, Maurine D. Miner, Erica Andersen-Nissen, Stephen C. De Rosa, Kelly E. Seaton, Georgia D. Tomaras, M. Juliana McElrath, Ann Ginsberg, and James G. Kublin

Subjects

Medicine (General), R5-920

Abstract

Background: Tuberculosis (TB) remains the leading cause of infectious disease-related death. Recently, a trial of BCG revaccination and vaccination with H4:IC31, a recombinant protein vaccine, in South African adolescents (Aeras C-040-404) showed efficacy in preventing sustained QuantiFERON (QFT) conversion, a proxy for Mycobacterium tuberculosis (M.tb) infection. A phase 1b trial of 84 South African adolescents was conducted, concurrent with Aeras C-040-404, to assess the safety and immunogenicity of H4:IC31, H56:IC31 and BCG revaccination, and to identify and optimize immune assays for identification of candidate correlates of protection in efficacy trials. Methods: Two doses of H4:IC31 and H56:IC31 vaccines were administered intramuscularly (IM) 56 days apart, and a single dose of BCG (2–8 × 105 CFU) was administered intradermally (ID). T-cell and antibody responses were measured using intracellular cytokine staining and binding antibody assays, respectively. Binding antibodies and CD4+/CD8+ T-cell responses to H4- and H56-matched antigens were measured in samples from all participants. The study was designed to characterize safety and immunogenicity and was not powered for group comparisons. (Clinicaltrials.gov NCT02378207). Findings: In total, 481 adolescents (mean age 13·9 years) were screened; 84 were enrolled (54% female). The vaccines were generally safe and well-tolerated, with no reported severe adverse events related to the study vaccines. H4:IC31 and H56:IC31 elicited CD4+ T cells recognizing vaccine-matched antigens and H4- and H56-specific IgG binding antibodies. The highest vaccine-induced CD4+ T-cell response rates were for those recognizing Ag85B in the H4:IC31 and H56:IC31 vaccinated groups. BCG revaccination elicited robust, polyfunctional BCG-specific CD4+ T cells, with no increase in H4- or H56-specific IgG binding antibodies. There were few antigen-specific CD8+ T-cell responses detected in any group. Interpretation: BCG revaccination administered as a single dose ID and both H4:IC31 and H56:IC31 administered as 2 doses IM had acceptable safety profiles in healthy, QFT-negative, previously BCG-vaccinated adolescents. Characterization of the assays and the immunogenicity of these vaccines may help to identify valuable markers of protection for upcoming immune correlates analyses of C-040-404 and future TB vaccine efficacy trials. Funding: NIAID and Aeras. Keywords: Mycobacterium tuberculosis, H4:IC31, H56:IC31, BCG

Published

2020

2. Safety and immunogenicity of a subtype C ALVAC-HIV (vCP2438) vaccine prime plus bivalent subtype C gp120 vaccine boost adjuvanted with MF59 or alum in healthy adults without HIV (HVTN 107): A phase 1/2a randomized trial.

Author

Zoe Moodie, Erica Andersen-Nissen, Nicole Grunenberg, One B Dintwe, Faatima Laher Omar, Jia J Kee, Linda-Gail Bekker, Fatima Laher, Nivashnee Naicker, Ilesh Jani, Nyaradzo M Mgodi, Portia Hunidzarira, Modulakgota Sebe, Maurine D Miner, Laura Polakowski, Shelly Ramirez, Michelle Nebergall, Simbarashe Takuva, Lerato Sikhosana, Jack Heptinstall, Kelly E Seaton, Stephen De Rosa, Carlos A Diazgranados, Marguerite Koutsoukos, Olivier Van Der Meeren, Susan W Barnett, Niranjan Kanesa-Thasan, James G Kublin, Georgia D Tomaras, M Juliana McElrath, Lawrence Corey, Kathryn Mngadi, Paul Goepfert, and HVTN 107 Protocol Team

Subjects

Medicine

Abstract

BackgroundAdjuvants are widely used to enhance and/or direct vaccine-induced immune responses yet rarely evaluated head-to-head. Our trial directly compared immune responses elicited by MF59 versus alum adjuvants in the RV144-like HIV vaccine regimen modified for the Southern African region. The RV144 trial of a recombinant canarypox vaccine vector expressing HIV env subtype B (ALVAC-HIV) prime followed by ALVAC-HIV plus a bivalent gp120 protein vaccine boost adjuvanted with alum is the only trial to have shown modest HIV vaccine efficacy. Data generated after RV144 suggested that use of MF59 adjuvant might allow lower protein doses to be used while maintaining robust immune responses. We evaluated safety and immunogenicity of an HIV recombinant canarypox vaccine vector expressing HIV env subtype C (ALVAC-HIV) prime followed by ALVAC-HIV plus a bivalent gp120 protein vaccine boost (gp120) adjuvanted with alum (ALVAC-HIV+gp120/alum) or MF59 (ALVAC-HIV+gp120/MF59) or unadjuvanted (ALVAC-HIV+gp120/no-adjuvant) and a regimen where ALVAC-HIV+gp120 adjuvanted with MF59 was used for the prime and boost (ALVAC-HIV+gp120/MF59 coadministration).Methods and findingsBetween June 19, 2017 and June 14, 2018, 132 healthy adults without HIV in South Africa, Zimbabwe, and Mozambique were randomized to receive intramuscularly: (1) 2 priming doses of ALVAC-HIV (months 0 and 1) followed by 3 booster doses of ALVAC-HIV+gp120/MF59 (months 3, 6, and 12), n = 36; (2) 2 priming doses of ALVAC-HIV (months 0 and 1) followed by 3 booster doses of ALVAC-HIV+gp120/alum (months 3, 6, and 12), n = 36; (3) 4 doses of ALVAC-HIV+gp120/MF59 coadministered (months 0, 1, 6, and 12), n = 36; or (4) 2 priming doses of ALVAC-HIV (months 0 and 1) followed by 3 booster doses of ALVAC-HIV+gp120/no adjuvant (months 3, 6, and 12), n = 24. Primary outcomes were safety and occurrence and mean fluorescence intensity (MFI) of vaccine-induced gp120-specific IgG and IgA binding antibodies at month 6.5. All vaccinations were safe and well-tolerated; increased alanine aminotransferase was the most frequent related adverse event, occurring in 2 (1.5%) participants (1 severe, 1 mild). At month 6.5, vaccine-specific gp120 IgG binding antibodies were detected in 100% of vaccinees for all 4 vaccine groups. No significant differences were seen in the occurrence and net MFI of vaccine-specific IgA responses between the ALVAC-HIV+gp120/MF59-prime-boost and ALVAC-HIV+gp120/alum-prime-boost groups or between the ALVAC-HIV+gp120/MF59-prime-boost and ALVAC-HIV+gp120/MF59 coadministration groups. Limitations were the relatively small sample size per group and lack of evaluation of higher gp120 doses.ConclusionsAlthough MF59 was expected to enhance immune responses, alum induced similar responses to MF59, suggesting that the choice between these adjuvants may not be critical for the ALVAC+gp120 regimen.Trial registrationHVTN 107 was registered with the South African National Clinical Trials Registry (DOH-27-0715-4894) and ClinicalTrials.gov (NCT03284710).

Published

2024

3. An outbreak of Candida spp. bloodstream infection in a tertiary care center in Bogotá, Colombia

Author

Carlos A. DiazGranados, Adriana Martinez, Ceneth Deaza, and Sandra Valderrama

Subjects

Candida, fungemia, disease outbreaks, developing countries, Colombia, Latin America, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

Several cases of Candida bloodstream infections were documented from June to October 2004 at a tertiary care center in Bogotá, Colombia. Since no cases of candidemia had occurred during the preceding four months, an outbreak was declared. As a result, a microbiological study, a revision of infection control practices and a case-control study were performed. In all, 18 cases of candidemia were ascertained. Parenteral nutrition (p=0.04), presence of a central line (p=0.03), and severity of illness (p=0.03) were associated with candidemia in bivariate analysis. Diverse Candida species were observed. Candida parapsilosis contamination was found in plastic containers used for transient intravenous (IV) medication storage at the bedside, plastic bags reused for the transportation of IV medicines and cotton used for disinfection of IV ports. Poor infection control practices were widely observed. The outbreak was controlled after elimination of plastic bags used for transportation, instauration of daily disinfection of IV medication containers, acquisition of sterile alcohol swabs for port disinfection and staff education. It was concluded that candidemia was associated with previously-described risk factors and that poor infection-control practices were likely responsible for the outbreak.

4. Safety and immune responses after a 12-month booster in healthy HIV-uninfected adults in HVTN 100 in South Africa: A randomized double-blind placebo-controlled trial of ALVAC-HIV (vCP2438) and bivalent subtype C gp120/MF59 vaccines.

Author

Fatima Laher, Zoe Moodie, Kristen W Cohen, Nicole Grunenberg, Linda-Gail Bekker, Mary Allen, Nicole Frahm, Nicole L Yates, Lynn Morris, Mookho Malahleha, Kathryn Mngadi, Brodie Daniels, Craig Innes, Kevin Saunders, Shannon Grant, Chenchen Yu, Peter B Gilbert, Sanjay Phogat, Carlos A DiazGranados, Marguerite Koutsoukos, Olivier Van Der Meeren, Carter Bentley, Nonhlanhla N Mkhize, Michael N Pensiero, Vijay L Mehra, James G Kublin, Lawrence Corey, David C Montefiori, Glenda E Gray, M Juliana McElrath, and Georgia D Tomaras

Subjects

Medicine

Abstract

BackgroundHVTN 100 evaluated the safety and immunogenicity of an HIV subtype C pox-protein vaccine regimen, investigating a 12-month booster to extend vaccine-induced immune responses.Methods and findingsA phase 1-2 randomized double-blind placebo-controlled trial enrolled 252 participants (210 vaccine/42 placebo; median age 23 years; 43% female) between 9 February 2015 and 26 May 2015. Vaccine recipients received ALVAC-HIV (vCP2438) alone at months 0 and 1 and with bivalent subtype C gp120/MF59 at months 3, 6, and 12. Antibody (IgG, IgG3 binding, and neutralizing) and CD4+ T-cell (expressing interferon-gamma, interleukin-2, and CD40 ligand) responses were evaluated at month 6.5 for all participants and at months 12, 12.5, and 18 for a randomly selected subset. The primary analysis compared IgG binding antibody (bAb) responses and CD4+ T-cell responses to 3 vaccine-matched antigens at peak (month 6.5 versus 12.5) and durability (month 12 versus 18) timepoints; IgG responses to CaseA2_gp70_V1V2.B, a primary correlate of risk in RV144, were also compared at these same timepoints. Secondary and exploratory analyses compared IgG3 bAb responses, IgG bAb breadth scores, neutralizing antibody (nAb) responses, antibody-dependent cellular phagocytosis, CD4+ polyfunctionality responses, and CD4+ memory sub-population responses at the same timepoints. Vaccines were generally safe and well tolerated. During the study, there were 2 deaths (both in the vaccine group and both unrelated to study products). Ten participants became HIV-infected during the trial, 7% (3/42) of placebo recipients and 3% (7/210) of vaccine recipients. All 8 serious adverse events were unrelated to study products. Less waning of immune responses was seen after the fifth vaccination than after the fourth, with higher antibody and cellular response rates at month 18 than at month 12: IgG bAb response rates to 1086.C V1V2, 21.0% versus 9.7% (difference = 11.3%, 95% CI = 0.6%-22.0%, P = 0.039), and ZM96.C V1V2, 21.0% versus 6.5% (difference = 14.5%, 95% CI = 4.1%-24.9%, P = 0.004). IgG bAb response rates to all 4 primary V1V2 antigens were higher 2 weeks after the fifth vaccination than 2 weeks after the fourth vaccination: 87.7% versus 75.4% (difference = 12.3%, 95% CI = 1.7%-22.9%, P = 0.022) for 1086.C V1V2, 86.0% versus 63.2% (difference = 22.8%, 95% CI = 9.1%-36.5%, P = 0.001) for TV1c8.2.C V1V2, 67.7% versus 44.6% (difference = 23.1%, 95% CI = 10.4%-35.7%, P < 0.001) for ZM96.C V1V2, and 81.5% versus 60.0% (difference = 21.5%, 95% CI = 7.6%-35.5%, P = 0.002) for CaseA2_gp70_V1V2.B. IgG bAb response rates to the 3 primary vaccine-matched gp120 antigens were all above 90% at both peak timepoints, with no significant differences seen, except a higher response rate to ZM96.C gp120 at month 18 versus month 12: 64.5% versus 1.6% (difference = 62.9%, 95% CI = 49.3%-76.5%, P < 0.001). CD4+ T-cell response rates were higher at month 18 than month 12 for all 3 primary vaccine-matched antigens: 47.3% versus 29.1% (difference = 18.2%, 95% CI = 2.9%-33.4%, P = 0.021) for 1086.C, 61.8% versus 38.2% (difference = 23.6%, 95% CI = 9.5%-37.8%, P = 0.001) for TV1.C, and 63.6% versus 41.8% (difference = 21.8%, 95% CI = 5.1%-38.5%, P = 0.007) for ZM96.C, with no significant differences seen at the peak timepoints. Limitations were that higher doses of gp120 were not evaluated, this study was not designed to investigate HIV prevention efficacy, and the clinical significance of the observed immunological effects is uncertain.ConclusionsIn this study, a 12-month booster of subtype C pox-protein vaccines restored immune responses, and slowed response decay compared to the 6-month vaccination.Trial registrationClinicalTrials.gov NCT02404311. South African National Clinical Trials Registry (SANCTR number: DOH--27-0215-4796).

Published

2020

5. Microneutralization assay titer correlates analysis in two phase 3 trials of the CYD-TDV tetravalent dengue vaccine in Asia and Latin America.

Author

Lindsay N Carpp, Youyi Fong, Matthew Bonaparte, Zoe Moodie, Michal Juraska, Ying Huang, Brenda Price, Yingying Zhuang, Jason Shao, Lingyi Zheng, Laurent Chambonneau, Robert Small, Saranya Sridhar, Carlos A DiazGranados, and Peter B Gilbert

Subjects

Medicine, Science

Abstract

We previously showed that Month 13 50% plaque reduction neutralization test (PRNT50) neutralizing antibody (nAb) titers against dengue virus (DENV) correlated with vaccine efficacy (VE) of CYD-TDV against symptomatic, virologically-confirmed dengue (VCD) in the CYD14 and CYD15 Phase 3 trials. While PRNT is the gold standard nAb assay, it is time-consuming and costly. We developed a next-generation high-throughput microneutralization (MN) assay and assessed its suitability for immune-correlates analyses and immuno-bridging applications. We analyzed MN and PRNT50 titers measured at baseline and Month 13 in a randomly sampled immunogenicity subset, and at Month 13 in nearly all VCD cases through Month 25. For each serotype, MN and PRNT50 titers showed high correlations, at both baseline and Month 13, with MN yielding a higher frequency of baseline-seronegatives. For both assays, Month 13 titer correlated inversely with VCD risk. Like PRNT50, high Month 13 MN titers were associated with high VE, and estimated VE increased with average Month 13 MN titer. We also studied each assay as a valid surrogate endpoint based on the Prentice criteria, which supported each assay as a valid surrogate for DENV-1 but only partially valid for DENV-2, -3, and -4. In addition, we applied Super-Learner to assess how well demographic, Month 13 MN, and/or Month 13 PRNT50 titers could predict Month 13-25 VCD outcome status; prediction was best when using demographic, MN, and PRNT50 information. We conclude that Month 13 MN titer performs comparably to Month 13 PRNT50 titer as a correlate of risk, correlate of vaccine efficacy, and surrogate endpoint. The MN assay could potentially be used to assess nAb titers in immunogenicity studies, immune-correlates studies, and immuno-bridging applications. Additional research would be needed for assessing the utility of MN titer in correlates analyses of other DENV endpoints and over longer follow-up periods.

Published

2020

6. Analysis of the HIV Vaccine Trials Network 702 Phase 2b–3 HIV-1 Vaccine Trial in South Africa Assessing RV144 Antibody and T-Cell Correlates of HIV-1 Acquisition Risk

Author

Zoe Moodie, One Dintwe, Sheetal Sawant, Doug Grove, Yunda Huang, Holly Janes, Jack Heptinstall, Faatima Laher Omar, Kristen Cohen, Stephen C De Rosa, Lu Zhang, Nicole L Yates, Marcella Sarzotti-Kelsoe, Kelly E Seaton, Fatima Laher, Linda Gail Bekker, Mookho Malahleha, Craig Innes, Sheetal Kassim, Nivashnee Naicker, Vaneshree Govender, Modulakgotla Sebe, Nishanta Singh, Philip Kotze, Erica Lazarus, Maphoshane Nchabeleng, Amy M Ward, William Brumskine, Thozama Dubula, April K Randhawa, Nicole Grunenberg, John Hural, Jia Jin Kee, David Benkeser, Yutong Jin, Lindsay N Carpp, Mary Allen, Patricia D’Souza, James Tartaglia, Carlos A DiazGranados, Marguerite Koutsoukos, Peter B Gilbert, James G Kublin, Lawrence Corey, Erica Andersen-Nissen, Glenda E Gray, Georgia D Tomaras, and M Juliana McElrath

Subjects

AIDS Vaccines, Male, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, South Africa, Infectious Diseases, Immunoglobulin G, HIV Seropositivity, Major Article, HIV-1, Humans, Immunology and Allergy, Female

Abstract

Background The ALVAC/gp120 + MF59 vaccines in the HIV Vaccine Trials Network (HVTN) 702 efficacy trial did not prevent human immunodeficiency virus-1 (HIV-1) acquisition. Vaccine-matched immunological endpoints that were correlates of HIV-1 acquisition risk in RV144 were measured in HVTN 702 and evaluated as correlates of HIV-1 acquisition. Methods Among 1893 HVTN 702 female vaccinees, 60 HIV-1–seropositive cases and 60 matched seronegative noncases were sampled. HIV-specific CD4+ T-cell and binding antibody responses were measured 2 weeks after fourth and fifth immunizations. Cox proportional hazards models assessed prespecified responses as predictors of HIV-1 acquisition. Results The HVTN 702 Env-specific CD4+ T-cell response rate was significantly higher than in RV144 (63% vs 40%, P = .03) with significantly lower IgG binding antibody response rate and magnitude to 1086.C V1V2 (67% vs 100%, P Conclusions HVTN 702 and RV144 had distinct immunogenicity profiles. However, both identified significant correlations (univariate or interaction) for IgG V1V2 and polyfunctional CD4+ T cells with HIV-1 acquisition. Clinical Trials Registration . NCT02968849.

Published

2022

7. Accuracy and efficacy of pre-dengue vaccination screening for previous dengue infection with a new dengue rapid diagnostic test: a retrospective analysis of phase 3 efficacy trials

Author

Stephen J, Savarino, Matthew, Bonaparte, Hao, Wang, Gustavo H, Dayan, Remi, Forrat, Ming, Zhu, Shekema, Hodge, Yasemin, Ataman-Önal, and Carlos A, DiazGranados

Subjects

Microbiology (medical), Biomedical Research, Vaccination, Dengue Vaccines, Dengue Virus, Antibodies, Viral, Microbiology, Dengue, Infectious Diseases, Immunoglobulin G, Virology, Humans, Vaccines, Combined, Retrospective Studies

Abstract

A dengue pre-vaccination test that is convenient, highly specific, and highly sensitive is still needed. The OnSite Dengue IgG rapid diagnostic test (RDT) is a new rapid diagnostic test specifically designed for pre-vaccination screening. We aimed to retrospectively assess the efficacy of a tetravalent dengue vaccine (CYD-TDV) in participants determined to be dengue seropositive by the OnSite IgG RDT and to evaluate assay performances.This was a complementary study using pre-vaccination samples from two CYD-TDV efficacy trials done in five countries in the Asia-Pacific region (NCT01373281) and five countries in Latin America (NCT01374516). Baseline dengue serostatus was determined by the OnSite IgG RDT on samples from the immunogenicity subsets of the two trials. In participants who were test positive, we calculated CYD-TDV vaccine efficacy against symptomatic virologically confirmed dengue (VCD) over 25 months, and against hospitalisation with VCD over 72 months of follow-up after the first vaccination. We used a reference algorithm to determine the reference dengue serostatus for each sample, and sensitivity and specificity of the OnSite IgG RDT were calculated. Analyses were done on the whole population (aged 2-16 years), and on those aged 6 years or older and those aged 9 years or older.Of 3983 participants in the immunogenicity subsets of the efficacy trials CYD14 and CYD15, 3962 had complete dengue reference test results enabling baseline serostatus classification and 3833 had sufficient serum samples remaining for evaluation with the OnSite IgG RDT. Of the samples tested, 2486 (64·9%) of 3833 were OnSite IgG RDT-positive. In participants aged 2-16 years who were OnSite IgG RDT-positive, vaccine efficacy was 84·1% (95% CI 71·6-91·1) against symptomatic VCD, and 69·2% (38·8-84·5) against hospitalisation with VCD, with similar findings in those aged 6 years or older and those aged 9 years or older. The OnSite IgG RDT showed very high sensitivity (91·1%, 89·9-92·1) and high specificity (92·8%, 91·2-94·2) in participants aged 2-16 years, with significantly higher specificity in those aged 9 years or older (96·6%, 94·9-97·8).The OnSite IgG RDT should provide a valuable tool for screening for previous dengue infection at the point of vaccination. In individuals who were OnSite IgG RDT-positive, the vaccine efficacy of CYD-TDV was high across all three age groups.Sanofi Pasteur.

Published

2022

8. Safety and immunogenicity of an AS03-adjuvanted SARS-CoV-2 recombinant protein vaccine (CoV2 preS dTM) in healthy adults: interim findings from a phase 2, randomised, dose-finding, multicentre study

Author

Saranya Sridhar, Arnel Joaquin, Matthew I Bonaparte, Agustin Bueso, Anne-Laure Chabanon, Aiying Chen, Roman M Chicz, David Diemert, Brandon J Essink, Bo Fu, Nicole A Grunenberg, Helene Janosczyk, Michael C Keefer, Doris M Rivera M, Ya Meng, Nelson L Michael, Sonal S Munsiff, Onyema Ogbuagu, Vanessa N Raabe, Randall Severance, Enrique Rivas, Natalya Romanyak, Nadine G Rouphael, Lode Schuerman, Lawrence D Sher, Stephen R Walsh, Judith White, Dalia von Barbier, Guy de Bruyn, Richard Canter, Marie-Helene Grillet, Maryam Keshtkar-Jahromi, Marguerite Koutsoukos, Denise Lopez, Roger Masotti, Sandra Mendoza, Catherine Moreau, Maria Angeles Ceregido, Shelly Ramirez, Ansoyta Said, Fernanda Tavares-Da-Silva, Jiayuan Shi, Tina Tong, John Treanor, Carlos A Diazgranados, and Stephen Savarino

Subjects

Adult, Vaccines, Synthetic, COVID-19 Vaccines, Adolescent, SARS-CoV-2, COVID-19, Articles, Middle Aged, Antibodies, Viral, Antibodies, Neutralizing, Recombinant Proteins, Young Adult, Immunogenicity, Vaccine, Infectious Diseases, Adjuvants, Immunologic, Double-Blind Method, Humans, Lactation, Female, Aged

Abstract

Background We evaluated our SARS-CoV-2 prefusion spike recombinant protein vaccine (CoV2 preS dTM) with different adjuvants, unadjuvanted, and in a one-injection and two-injection dosing schedule in a previous phase 1–2 study. Based on interim results from that study, we selected a two-injection schedule and the AS03 adjuvant for further clinical development. However, lower than expected antibody responses, particularly in older adults, and higher than expected reactogenicity after the second vaccination were observed. In the current study, we evaluated the safety and immunogenicity of an optimised formulation of CoV2 preS dTM adjuvanted with AS03 to inform progression to phase 3 clinical trial. Methods This phase 2, randomised, parallel-group, dose-ranging study was done in adults (≥18 years old), including those with pre-existing medical conditions, those who were immunocompromised (except those with recent organ transplant or chemotherapy) and those with a potentially increased risk for severe COVID-19, at 20 clinical research centres in the USA and Honduras. Women who were pregnant or lactating or, for those of childbearing potential, not using an effective method of contraception or abstinence, and those who had received a COVID-19 vaccine, were excluded. Participants were randomly assigned (1:1:1) using an interactive response technology system, with stratification by age (18–59 years and ≥60 years), rapid serodiagnostic test result (positive or negative), and high-risk medical conditions (yes or no), to receive two injections (day 1 and day 22) of 5 7mu;g (low dose), 10 7mu;g (medium dose), or 15 7mu;g (high dose) CoV2 preS dTM antigen with fixed AS03 content. All participants and outcome assessors were masked to group assignment; unmasked study staff involved in vaccine preparation were not involved in safety outcome assessments. All laboratory staff performing the assays were masked to treatment. The primary safety objective was to describe the safety profile in all participants, for each candidate vaccine formulation. Safety endpoints were evaluated for all randomised participants who received at least one dose of the study vaccine (safety analysis set), and are presented here for the interim study period (up to day 43). The primary immunogenicity objective was to describe the neutralising antibody titres to the D614G variant 14 days after the second vaccination (day 36) in participants who were SARS-CoV-2 naive who received both injections, provided samples at day 1 and day 36, did not have protocol deviations, and did not receive an authorised COVID-19 vaccine before day 36. Neutralising antibodies were measured using a pseudovirus neutralisation assay and are presented here up to 14 days after the second dose. As a secondary immunogenicity objective, we assessed neutralising antibodies in non-naive participants. This trial is registered with ClinicalTrials.gov (NCT04762680) and is closed to new participants for the cohort reported here. Findings Of 722 participants enrolled and randomly assigned between Feb 24, 2021, and March 8, 2021, 721 received at least one injection (low dose=240, medium dose=239, and high dose=242). The proportion of participants reporting at least one solicited adverse reaction (injection site or systemic) in the first 7 days after any vaccination was similar between treatment groups (217 [91%] of 238 in the low-dose group, 213 [90%] of 237 in the medium-dose group, and 218 [91%] of 239 in the high-dose group); these adverse reactions were transient, were mostly mild to moderate in intensity, and occurred at a higher frequency and intensity after the second vaccination. Four participants reported immediate unsolicited adverse events; two (one each in the low-dose group and medium-dose group) were considered by the investigators to be vaccine related and two (one each in the low-dose and high-dose groups) were considered unrelated. Five participants reported seven vaccine-related medically attended adverse events (two in the low-dose group, one in the medium-dose group, and four in the high-dose group). No vaccine-related serious adverse events and no adverse events of special interest were reported. Among participants naive to SARS-CoV-2 at day 36, 158 (98%) of 162 in the low-dose group, 166 (99%) of 168 in the medium-dose group, and 163 (98%) of 166 in the high-dose group had at least a two-fold increase in neutralising antibody titres to the D614G variant from baseline. Neutralising antibody geometric mean titres (GMTs) at day 36 for participants who were naive were 2189 (95% CI 1744–2746) for the low-dose group, 2269 (1792–2873) for the medium-dose group, and 2895 (2294–3654) for the high-dose group. GMT ratios (day 36: day 1) were 107 (95% CI 85–135) in the low-dose group, 110 (87–140) in the medium-dose group, and 141 (111–179) in the high-dose group. Neutralising antibody titres in non-naive adults 21 days after one injection tended to be higher than titres after two injections in adults who were naive, with GMTs 21 days after one injection for participants who were non-naive being 3143 (95% CI 836–11 815) in the low-dose group, 2338 (593–9226) in the medium-dose group, and 7069 (1361–36 725) in the high-dose group. Interpretation Two injections of CoV2 preS dTM-AS03 showed acceptable safety and reactogenicity, and robust immunogenicity in adults who were SARS-CoV-2 naive and non-naive. These results supported progression to phase 3 evaluation of the 10 7mu;g antigen dose for primary vaccination and a 5 7mu;g antigen dose for booster vaccination. Funding Sanofi Pasteur and Biomedical Advanced Research and Development Authority.

Published

2022

9. Efficacy of a bivalent (D614 + B.1.351) SARS-CoV-2 Protein Vaccine

Author

Gustavo H, Dayan, Nadine, Rouphael, Stephen R, Walsh, Aiying, Chen, Nicole, Grunenberg, Mary, Allen, Johannes, Antony, Kwaku Poku, Asante, Amit Suresh, Bhate, Tatiana, Beresnev, Matthew I, Bonaparte, Maria, Angeles Ceregido, Dmytro, Dobrianskyi, Bo, Fu, Marie-Helene, Grillet, Maryam, Keshtkar-Jahromi, Michal, Juraska, Jia Jin, Kee, Hannah, Kibuuka, Marguerite, Koutsoukos, Roger, Masotti, Nelson L, Michael, Humberto, Reynales, Merlin L, Robb, Sandra M, Villagómez Martínez, Fredrick, Sawe, Lode, Schuerman, Tina, Tong, John, Treanor, T Anh, Wartel, Carlos A, Diazgranados, Roman M, Chicz, Sanjay, Gurunathan, Stephen, Savarino, and Saranya, Sridhar

Abstract

BackgroundCOVID-19 vaccines with alternative strain compositions are needed to provide broad protection against newly emergent SARS-CoV-2 variants of concern.MethodsWe conducted a global Phase 3, multi-stage efficacy study (NCT04904549) among adults aged ≥18 years. Participants were randomized 1:1 to receive two intramuscular injections 21 days apart of a bivalent SARS-CoV-2 recombinant protein vaccine with AS03-adjuvant (5 μg of ancestral (D614) and 5 μg of B.1.351 [beta] variant spike protein) or placebo. Symptomatic COVID-19 was defined as laboratory-confirmed COVID-19 with COVID-19-like illness (CLI) symptoms. The primary efficacy endpoint was the prevention of symptomatic COVID-19 ≥14 days after the second injection (post-dose 2 [PD2]).ResultsBetween 19 Oct 2021 and 15 Feb 2022, 12,924 participants received ≥1 study injection. 75% of participants were SARS-CoV-2 non-naïve. 11,416 participants received both study injections (efficacy-evaluable population [vaccine, n=5,736; placebo, n=5,680]). Up to 15 March 2022, 121 symptomatic COVID-19 cases were reported (32 in the vaccine group and 89 in the placebo group) ≥14 days PD2 with a vaccine efficacy (VE) of 64.7% (95% confidence interval [CI] 46.6; 77.2%). VE was 75.1% (95% CI 56.3; 86.6%) in non-naïve and 30.9% (95% CI -39.3; 66.7%) in naïve participants. Viral genome sequencing identified the infecting strain in 68 cases (Omicron [BA.1 and BA.2 subvariants]: 63; Delta: 4; Omicron and Delta: 1). The vaccine was well-tolerated and had an acceptable safety profile.ConclusionsA bivalent vaccine conferred heterologous protection against symptomatic infection with newly emergent Omicron (BA.1 and BA.2) in non-naïve adults 18–59 years of age.ClinicalTrials.govNCT04904549

Published

2022

10. Immunogenicity and safety of simplified vaccination schedules for the CYD-TDV dengue vaccine in healthy individuals aged 9–50 years (CYD65): a randomised, controlled, phase 2, non-inferiority study

Author

Jenny Carolina Ramírez, Carlos A. DiazGranados, Andrey Rojas, Diana Leticia Coronel-MartÍnez, Isabel Cristina Ramirez, Eduardo López-Medina, María Cecilia Montalbán, Maria Liza Antoinette Gonzales, Sunny Sun, Fernando Noriega, Hao Wang, Stephen Savarino, Juliana Park, Gustavo H. Dayan, Maria Rosario Capeding, Andrés Angelo Cadena Bonfanti, Zhenghong Chen, Matthew Bonaparte, Mae Ann Verdan, and Betzana Zambrano

Subjects

Adult, Male, Serotype, medicine.medical_specialty, Adolescent, 030231 tropical medicine, Dengue Vaccines, Dengue virus, Antibodies, Viral, Vaccines, Attenuated, Placebo, medicine.disease_cause, Dengue fever, Dengue, Young Adult, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Internal medicine, Humans, Medicine, 030212 general & internal medicine, Child, Immunization Schedule, Dengue vaccine, Reactogenicity, business.industry, Dengue Virus, Middle Aged, medicine.disease, Antibodies, Neutralizing, Healthy Volunteers, Vaccination, Regimen, Infectious Diseases, Female, business

Abstract

Summary Background Three doses of the licensed tetravalent dengue vaccine CYD-TDV (Dengvaxia, Sanofi Pasteur, Lyon France) are immunogenic and effective against symptomatic dengue in individuals aged 9 years and older who are dengue seropositive. Previous trials have provided some evidence that antibody responses elicited after just one dose or two doses of CYD-TDV might be similar to those elicited after three doses. We compared antibody responses following one-dose, two-dose, and three-dose vaccination regimens in individuals who were dengue seropositive at baseline up to 1 year after the last injection. Methods In this randomised, controlled, phase 2, non-inferiority study (CYD65), healthy individuals aged 9–50 years were recruited from the community in three sites in Colombia and three sites in the Philippines. Participants were randomly assigned (1:1:1), using a permuted block method with stratification by site and age group, to receive, at 6-month intervals (on day 0, month 6, and month 12), three doses of CYD-TDV (three-dose group), one dose of placebo (on day 0) and two doses of CYD-TDV (at months 6 and 12; two-dose group), or two doses of placebo (on day 0 and month 6) and one dose of CYD-TDV (at month 12; one-dose group). Each dose of CYD-TDV was 0·5 mL, administered subcutaneously into the deltoid of the upper arm. Participants, study staff, investigators, and the funder were masked to group assignment. The co-primary endpoints were geometric mean titres (GMTs) of neutralising antibodies against each dengue virus serotype at 28 days and 1 year after the last vaccine injection. After a protocol amendment during the conduct of the study, the original co-primary objectives of non-inferiority of the one-dose and two-dose groups to the three-dose group were altered to include non-inferiority of the two-dose group to the three-dose group only, to be assessed in individuals who were dengue seropositive at baseline. Non-inferiority was shown if the lower limit of the 95% CI for the ratio of GMTs (GMR) at 28 days and 1 year between groups was more than 0·5 for each serotype. The analysis of the coprimary objectives was done in the per-protocol analysis dataset, which included all participants who had been vaccinated, had no protocol deviations, and had a valid serology test result for at least one dengue serotype at 28 days after the third injection. Safety was assessed throughout in all participants who received at least one injection of study drug, regardless of serostatus. This trial is registered with ClinicalTrials.gov , NCT02628444 , and is closed to accrual. Findings Between May 2, 2016, and Sept 16, 2016, we recruited and enrolled 1050 individuals, of whom 1048 received at least one injection and 993 had at least one blood sample taken (full-analysis dataset; 333 in three-dose group, 328 in two-dose group, and 332 in one-dose group). 860 (86·6%) of 993 participants in the full-analysis dataset were dengue seropositive at baseline. Non-inferiority (two dose vs three dose) was shown for each serotype at both 28 days and 1 year among dengue-seropositive participants (number of participants assessed: 272 [two-dose group], 265 [three-dose group] at 28 days; and 190 [two-dose group], 185 [three-dose group] at 1 year). At 28 days after the last injection, neutralising antibody GMTs were 899 (95% CI 752–1075) in the two-dose group versus 822 (700–964) in the three dose group against dengue serotype 1 (GMR 1·09 [95% CI 0·86–1·39]); 869 (754–1002) versus 875 (770–995) against serotype 2 (GMR 0·99 [0·82–1·20]); 599 (524–685) versus 610 (535–694) against serotype 3 (GMR 0·98 [0·82–1·18]); and 510 (453–575) versus 531 (470–601) against serotype 4 (GMR 0·96 [0·81–1·14]). At year 1, GMTs had decreased but remained above baseline for all serotypes: 504 (95% CI 403–630) in the two-dose group versus 490 (398–604) in the three-dose group against serotype 1 (GMR 1·03 [0·76–1·40]); 737 (611–888) versus 821 (704–957) against serotype 2 (GMR 0·90 [0·71–1·14]); 437 (368–519) versus 477 (405–561) against serotype 3 (GMR 0·92 [0·72–1·16]); and 238 (205–277) versus 270 (235–310) against serotype 4 (GMR 0·88 [0·72–1·09]). Reactogenicity profiles were similar across treatment groups. Most unsolicited adverse events after any injection were non-serious and systemic in nature. During the study, 60 serious adverse events were reported in 58 participants (14 in three-dose group, 26 in two-dose group, 18 in one-dose group), mostly infection and infestations or injury, poisoning, and procedural complications. No serious adverse events of special interest or admissions to hospital for dengue occurred. Two deaths occurred, unrelated to study treatment. Interpretation A two-dose CYD-TDV regimen might be an alternative to the licensed three-dose regimen in individuals who are dengue seropositive at baseline and aged 9 years and older. Vaccination with a reduced number of doses could lead to improved vaccine compliance and coverage, especially in low-resource settings. Funding Sanofi Pasteur.

Published

2021

11. Immunobridging efficacy of a tetravalent dengue vaccine against dengue and against hospitalized dengue from children/adolescents to adults in highly endemic countries

Author

Zoe Moodie, Lindsay N. Carpp, Gustavo H. Dayan, Peter B. Gilbert, Ying Huang, Carlos A. DiazGranados, Youyi Fong, Diana Coronel, Laurent Chambonneau, and Michal Juraska

Subjects

Adult, Serotype, medicine.medical_specialty, Adolescent, 030231 tropical medicine, Dengue Vaccines, Antibodies, Viral, Vaccines, Attenuated, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Plaque reduction neutralization test, Internal medicine, Humans, Medicine, Vaccines, Combined, 030212 general & internal medicine, Child, Dengue vaccine, business.industry, Surrogate endpoint, Public Health, Environmental and Occupational Health, General Medicine, Dengue Virus, medicine.disease, Vaccine efficacy, Antibodies, Neutralizing, Titer, Infectious Diseases, Early adolescents, Original Article, Parasitology, business

Abstract

BackgroundThe recombinant tetravalent live-attenuated dengue vaccine based on the YF 17D vaccine virus backbone (CYD-TDV) demonstrated vaccine efficacy (VE) against symptomatic, virologically confirmed dengue of any serotype from month 13 to month 25 (VCD-DENV-AnyM13→M25) in the CYD14 (2–14-y-olds) and CYD15 (9–16-y-olds) phase 3 trials. Fifty percent plaque reduction neutralization test (PRNT50) titers are a potential surrogate for immunobridging VE to adults.MethodsUsing PRNT50 calibration datasets, we applied immunobridging approaches using baseline and/or M13 PRNT50 titers to estimate VE against VCD-DENV-AnyM0→M25 and against hospitalized VCD (HVCD)-DENV-AnyM0→M72 in hypothetical 18–45-y-old and 46–50-y-old CYD14 and CYD15 cohorts.ResultsBaseline and M13 geometric mean PRNT50 titers were greater in 18–45-y-olds and in 46–50-y-olds vs 9–16-y-olds for most comparisons. Estimated VE (95% CIs against VCD-DENV-AnyM0→M25 ranged from 75.3% to 90.9% (52.5% to 100%) for 18–45-y-olds and 74.8% to 92.0% (53.4% to 100%) for 46–50-y-olds. Estimated VE (95% CIs) against HVCD-DENV-AnyM0→M72 ranged from 58.8% to 78.1% (40.9 to 98.9%) for 18–45-y-olds and 57.2% to 78.4% (40.5 to 97.6%) for 46–50-y-olds. Corresponding predictions among baseline-seropositive individuals yielded comparable or higher VE estimates.ConclusionsVE M0→M25 against DENV-Any and VE against HVCD-DENV-AnyM0→M72 are both expected to be higher in 18–45 and 46–50-y-olds vs CYD14 and CYD15 9–16-y-olds.

Published

2020

12. CYD Tetravalent Dengue Vaccine Performance by Baseline Immune Profile (Monotypic/Multitypic) in Dengue-Seropositive Individuals

Author

Saranya Sridhar, Stephen Savarino, Matthew Bonaparte, Carlos A. DiazGranados, Gustavo H. Dayan, Edith Langevin, Remi Forrat, and Tifany Machabert

Subjects

Microbiology (medical), medicine.medical_specialty, 030231 tropical medicine, Dengue Vaccines, Antibodies, Viral, Placebo, Lower risk, CYD15, CYD14, Dengue fever, Dengue, 03 medical and health sciences, monotypic, 0302 clinical medicine, Plaque reduction neutralization test, Internal medicine, medicine, Humans, Vaccines, Combined, 030212 general & internal medicine, Dengue vaccine, business.industry, Immunogenicity, Absolute risk reduction, Dengue Virus, Vaccine efficacy, medicine.disease, Major Articles and Commentaries, AcademicSubjects/MED00290, Infectious Diseases, multitypic, business

Abstract

Background The immune profile of dengue-experienced individuals is a determinant of dengue reinfection severity risk. Individuals with a single prior dengue infection (monotypic) are at highest risk for severe disease, while individuals with ≥ 2 prior dengue infections (multitypic) are at lower risk. The tetravalent dengue vaccine (CYD-TDV) has shown efficacy in the prevention of dengue in individuals with prior dengue infection. We estimated efficacy in individuals with monotypic or multitypic immune profiles. Methods Participants enrolled in the immunogenicity subsets of 2 randomized placebo-controlled phase 3 studies (CYD14, NCT01373281; CYD15, NCT01374516) were classified as either monotypic or multitypic, based on measured baseline dengue plaque reduction neutralization test. Vaccine efficacy (VE) against symptomatic virologically confirmed dengue (VCD) was assessed over 25 months and against VCD hospitalization over 6 years. Results Of 3927 participants in the immunogenicity subsets, 496 and 257 in the CYD-TDV and placebo groups, respectively, were classified as monotypic immune, and 1227 and 612, respectively, as multitypic immune. VE against symptomatic VCD was 77.4% (95% CI, 56.4%–88.2%) for monotypic and 89.2% (95% CI, 71.5%–95.9%) for multitypic profiles, with corresponding absolute risk reductions (ARRs) of 4.48% (95% CI, 2.32%–6.65%) for monotypics and 1.67% (95% CI, .89%–2.46%) for multitypics. VE against hospitalized VCD was 75.3% (95% CI, 42.7%–90.2%) in monotypics and 81.2% (95% CI, 21.7%–96.8%) in multitypics, with ARRs of 0.95% (95% CI, .37%–1.53%) for monotypics and 0.18% (95% CI, .02%–.34%) for multitypics. Conclusions CYD-TDV benefits individuals with monotypic and multitypic immune profiles. Larger public health benefit is expected to derive from the protection of individuals with a monotypic immune profile., Dengue vaccine efficacy was assessed by participant seropositivity immune profile: monotypic (1 dengue serotype) or multitypic (≥ 2 dengue serotypes). Protection against symptomatic dengue and dengue hospitalization was observed for both monotypic and multitypic immune profiles.

Published

2020

13. Safety and immunogenicity of a SARS-CoV-2 recombinant protein vaccine with AS03 adjuvant in healthy adults: interim findings from a phase 2, randomised, dose-finding, multi-centre study

Author

Agustin Bueso, John J. Treanor, Maria Angeles Ceregido, Shelly Ramirez, Aiying Chen, Matthew Bonaparte, Saranya Sridhar, David Diemert, Helene Janosczyk, Sonal S. Munsiff, Guy de Bruyn, Ya Meng, Marie-Helene Grillet, Catherine Moreau, Onyema Ogbuagu, Roger Masotti, Marguerite Koutsoukos, Fernanda Tavares-Da-Silva, Carlos A. DiazGranados, Denise Lopez, Doris M Rivera M, Brandon Essink, Stephen R. Walsh, Jiayuan Shi, Anne-Laure Chabanon, Nicole Grunenberg, Richard Canter, Vanessa Raabe, Ansoyta Said, Dalia von Barbier, Joaquin Arnel, Enrique Rivas, Bo Fu, Lode Schuerman, Nadine Rouphael, Natalya Romanyak, Michael C. Keefer, Maryam Keshtkar-Jahromi, Lawrence D Sher, Sandra Mendoza, Nelson L. Michael, Judith M. White, Tina Tong, Roman Chicz, Randall Severance, and Stephen Savarino

Subjects

medicine.medical_specialty, Reactogenicity, biology, business.industry, Immunogenicity, medicine.medical_treatment, Antigen, Internal medicine, Interim, medicine, biology.protein, AS03, Antibody, Adverse effect, business, Adjuvant

Abstract

SummaryBackgroundThis study evaluated the safety and immunogenicity of an AS03-adjuvanted SARS-CoV-2 recombinant protein candidate vaccine, CoV2 preS dTM.MethodsThis Phase 2, modified double-blind, parallel-group study (NCT04762680) was conducted in adults, including those at increased risk of severe COVID-19. Participants were randomised 1:1:1, stratified by age (18–59/≥60 years), rapid serodiagnostic test (positive/negative) and high-risk medical conditions (yes/no), to receive two injections (day [D]1 and D22) of 5μg, 10μg or 15μg of CoV2 preS dTM antigen with fixed AS03 content. Interim safety and reactogenicity results (to D43) and neutralising antibodies (NAbs) against the D614G variant are presented (primary objectives).FindingsOf 722 participants enrolled and randomised between 24 February and 8 March 2021, 721 received ≥1 injections (5μg, n=240; 10μg, n=239; 15μg, n=242). Four participants reported unsolicited immediate adverse events (AEs), two were vaccine-related (investigator assessment). Five participants reported seven vaccine-related medically-attended AEs. No vaccine-related serious AEs and no AEs of special interest were reported. Solicited reactions (local and systemic) were reported at similar frequencies between study groups; these were mostly mild to moderate and transient, with higher frequency and intensity post-injection 2 than post-injection 1. In SARS-CoV-2 naïve participants at D36, 96·9%, 97.0% and 97·6% of participants had ≥4-fold-rise in NAb titres from baseline in the 5μg-, 10μg- and 15μg-dose groups, respectively. NAb titres increased with antigen dose in younger (GMTs: 2954, 3951 and 5142 for 5μg-, 10μg- and 15μg-dose groups) but not older adults (GMTs: 1628, 1393 and 1736, respectively). NAb titres in non-naïve adults after one injection were higher than titres after two injections in naïve adults.InterpretationTwo injections of CoV2 preS dTM-AS03 demonstrated acceptable safety and reactogenicity, and robust immunogenicity in SARS-CoV-2 naïve and non-naïve adults. These results informed antigen dose selection for progression to Phase 3 evaluation of primary and booster vaccination.

Published

2021

14. Safety and immunogenicity of SARS-CoV-2 recombinant protein vaccine formulations in healthy adults: interim results of a randomised, placebo-controlled, phase 1-2, dose-ranging study

Author

Murray A Kimmel, Guy de Bruyn, Anne-Laure Chabanon, Ian Frank, Helene Janosczyk, Fernanda Tavares-Da-Silva, Jon Smith, Owen Haney, Matthew Davis, Roger Masotti, Brandon Essink, Marguerite Koutsoukos, Carlos A. DiazGranados, Michael C. Keefer, Lawrence D Sher, Howard J. Schwartz, Bo Fu, Lode Schuerman, Sanjay Gurunathan, Matthew Bonaparte, Stephen Savarino, and Paul A. Goepfert

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, COVID-19 Vaccines, Placebo, Antibodies, Viral, law.invention, 03 medical and health sciences, 0302 clinical medicine, Immunogenicity, Vaccine, Randomized controlled trial, Adjuvants, Immunologic, Double-Blind Method, law, Internal medicine, Medicine, Humans, 030212 general & internal medicine, AS03, Adverse effect, Reactogenicity, business.industry, SARS-CoV-2, COVID-19, Articles, Middle Aged, Dose-ranging study, Interim analysis, Antibodies, Neutralizing, Recombinant Proteins, United States, Vaccination, 030104 developmental biology, Infectious Diseases, Spike Glycoprotein, Coronavirus, Female, business

Abstract

BACKGROUND: CoV2 preS dTM is a stabilised pre-fusion spike protein vaccine produced in a baculovirus expression system being developed against SARS-CoV-2. We present interim safety and immunogenicity results of the first-in-human study of the CoV2 preS dTM vaccine with two different adjuvant formulations. METHODS: This phase 1-2, randomised, double-blind study is being done in healthy, SARS-CoV-2-seronegative adults in ten clinical research centres in the USA. Participants were stratified by age (18-49 years and ≥50 years) and randomly assigned using an interactive response technology system with block randomisation (blocks of varying size) to receive one dose (on day 1) or two doses (on days 1 and 22) of placebo or candidate vaccine, containing low-dose (effective dose 1·3 µg) or high-dose (2·6 µg) antigen with adjuvant AF03 (Sanofi Pasteur) or AS03 (GlaxoSmithKline) or unadjuvanted high-dose antigen (18-49 years only). Primary endpoints were safety, assessed up to day 43, and immunogenicity, measured as SARS-C0V-2 neutralising antibodies (geometric mean titres), assessed on days 1, 22, and 36 serum samples. Safety was assessed according to treatment received in the safety analysis set, which included all randomly assigned participants who received at least one dose. Neutralising antibody titres were assessed in the per-protocol analysis set for immunogenicity, which included participants who received at least one dose, met all inclusion and exclusion criteria, had no protocol deviation, had negative results in the neutralisation test at baseline, and had at least one valid post-dose serology sample. This planned interim analysis reports data up to 43 days after the first vaccination; participants in the trial will be followed up for 12 months after the last study injection. This trial is registered with ClinicalTrials.gov, NCT04537208, and is ongoing. FINDINGS: Between Sept 3 and Sept 29, 2020, 441 individuals (299 aged 18-49 years and 142 aged ≥50 years) were randomly assigned to one of the 11 treatment groups. The interim safety analyses included 439 (>99%) of 441 randomly assigned participants (299 aged 18-49 years and 140 aged ≥50 years). Neutralising antibody titres were analysed in 326 (74%) of 441 participants (235 [79%] of 299 aged 18-49 years and 91 [64%] of 142 aged ≥50 years). There were no vaccine-related unsolicited immediate adverse events, serious adverse events, medically attended adverse events classified as severe, or adverse events of special interest. Among all study participants, solicited local and systemic reactions of any grade after two vaccine doses were reported in 81% (95% CI 61-93; 21 of 26) of participants in the low-dose plus AF03 group, 93% (84-97; 74 of 80) in the low-dose plus AS03 group, 89% (70-98; 23 of 26) in the high-dose plus AF03 group, 95% (88-99; 81 of 85) in the high-dose plus AS03 group, 29% (10-56; five of 17) in the unadjuvanted high-dose group, and 21% (8-40; six of 29) in the placebo group. A single vaccine dose did not generate neutralising antibody titres above placebo levels in any group at days 22 or 36. Among participants aged 18-49 years, neutralising antibody titres after two vaccine doses were 13·1 (95% CI 6·40-26·9) in the low-dose plus AF03 group, 20·5 (13·1-32·1) in the low-dose plus AS03 group, 43·2 (20·6-90·4) in the high-dose plus AF03 group, 75·1 (50·5-112·0) in the high-dose plus AS03 group, 5·00 (not calculated) in the unadjuvanted high-dose group, and 5·00 (not calculated) in the placebo group. Among participants aged 50 years or older, neutralising antibody titres after two vaccine doses were 8·62 (1·90-39·0) in the low-dose plus AF03 group, 12·9 (7·09-23·4) in the low-dose plus AS03 group, 12·3 (4·35-35·0) in the high-dose plus AF03 group, 52·3 (25·3-108·0) in the high-dose plus AS03 group, and 5·00 (not calculated) in the placebo group. INTERPRETATION: The lower than expected immune responses, especially in the older age groups, and the high reactogenicity after dose two were probably due to higher than anticipated host-cell protein content and lower than planned antigen doses in the formulations tested, which was discovered during characterisation studies on the final bulk drug substance. Further development of the AS03-adjuvanted candidate vaccine will focus on identifying the optimal antigen formulation and dose. FUNDING: Sanofi Pasteur and Biomedical Advanced Research and Development Authority.

Published

2021

15. Safety and immunogenicity of SARS-CoV-2 recombinant protein vaccine formulations in healthy adults: a randomised, placebo-controlled, dose-ranging study

Author

Roger Masotti, Helene Janosczyk, Howard J. Schwartz, Anne-Laure Chabanon, Owen Haney, Lawrence D Sher, Bo Fu, Lode Schuerman, Marguerite Koutsoukos, Guy deBruyn, Carlos A. DiazGranados, Brandon Essink, Michael C. Keefer, Stephen Savarino, Matthew Davis, Ian Frank, Jon Smith, Murray A Kimmel, Fernanda Tavares-Da-Silva, Sanjay Gurunathan, Matthew Bonaparte, and Paul A. Goepfert

Subjects

medicine.medical_specialty, Reactogenicity, business.industry, medicine.medical_treatment, Immunogenicity, Placebo, Dose-ranging study, Effective dose (pharmacology), Antigen, Internal medicine, medicine, AS03, business, Adjuvant

Abstract

BackgroundEffective vaccines against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are urgently needed. CoV2 preS dTM is a stabilised pre-fusion S protein vaccine produced in a baculovirus expression system. We present interim safety and immunogenicity results of the first-in-human study of the CoV2 preS dTM vaccine with two different adjuvant formulations.MethodsThis Phase I/II, randomised, double-blind study (NCT04537208) is being conducted in healthy, SARS-CoV-2-seronegative adults in the USA. Participants were stratified by age (18–49 and ≥50 years) and randomised to receive one (on Day[D]1) or two doses (D1, D22) of placebo or candidate vaccine, containing: low-dose (LD, effective dose 1.3 µg) or high-dose (HD, 2.6 µg) antigen with adjuvant AF03 (Sanofi Pasteur) or AS03 (GlaxoSmithKline); or unadjuvanted HD (18–49 years only). Safety was assessed up to D43. SARS-CoV-2 neutralising and binding antibody profiles were assessed in D1, D22 and D36 serum samples.FindingsThe interim safety analyses included 439/441 randomised participants. There were no related unsolicited immediate AEs, serious AEs, medically attended AEs classified as severe, or AE of special interest. More grade 3 solicited reactions were reported than expected after the second dose in the adjuvanted vaccine groups. Neutralising and binding antibody responses after two vaccine doses were higher in adjuvanted versus unadjuvanted groups, in AS03-versus AF03-adjuvanted groups, in HD versus LD groups, and in younger versus older age strata.InterpretationThe lower than expected immune responses, especially in the older age stratum, and the higher than anticipated reactogenicity post dose 2 were likely due to a higher than anticipated host cell protein content and lower than planned antigen dose in the clinical material. Further development of the AS03-adjuvanted candidate vaccine will focus on identifying the optimal antigen formulation and dose.

Published

2021

16. Zika and Dengue Interactions in the Context of a Large Dengue Vaccine Clinical Trial in Latin America

Author

Yukun Wu, José Luis Arredondo, Carlos A. DiazGranados, Margarita Cortés, Fernando Noriega, Betzana Zambrano, Kleber Giovanni Luz, Doris Maribel Rivera, Carmen Deseda, Stephen Savarino, Humberto Reynales, Gustavo H. Dayan, Edith Langevin, and Matthew Bonaparte

Subjects

Male, Adolescent, 030231 tropical medicine, Context (language use), Dengue Vaccines, Antibodies, Viral, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Plaque reduction neutralization test, Virology, Medicine, Humans, Neutralizing antibody, Child, Epidemics, Dengue vaccine, biology, business.industry, Coinfection, Zika Virus Infection, Articles, medicine.disease, Vaccine efficacy, Antibodies, Neutralizing, Vaccination, Infectious Diseases, Latin America, biology.protein, Parasitology, Female, business, Serostatus

Abstract

A phase III dengue vaccine trial including 9- to 16-year-olds in Latin America (NCT01374516) was ongoing at the time of a Zika outbreak. We explored interactions between dengue and Zika, in the context of dengue vaccination. Symptomatic virologically confirmed Zika (VCZ) was evaluated using acute-phase sera from febrile participants (January 2013–March 2018). Neutralizing antibody geometric mean titers (GMTs) were evaluated pre- and post-Zika outbreak (months 25 and 72) in 2,000 randomly selected participants. Baseline dengue serostatus was determined using the plaque reduction neutralization test or inferred post hoc using nonstructural protein 1 IgG ELISA at M13 (case–cohort analysis). Vaccine efficacy against VCZ and serologically suspected Zika (SSZ) was estimated. Overall, 239/10,157 (2.4%) acute-phase samples were VCZ positive during the study. Dengue vaccine efficacy against VCZ was 27.8% (95% CI: 0.3; 47.7) among baseline dengue-seropositive participants. No vaccine effect was evident against SSZ. Zika antibody GMTs increased from pre- to post-Zika epidemic, with smaller increases observed for participants who were dengue seropositive at baseline than for those who were dengue seronegative: post-/pre-Zika GMT ratios for baseline dengue-seropositive participants were 21.5 (vaccine group) and 30.8 (placebo); and for dengue seronegatives, 88.1 and 89.5, respectively. Dengue antibody GMTs post-Zika were higher in dengue vaccine and placebo recipients with SSZ than those without SSZ in both dengue seropositives and seronegatives. Dengue vaccine did not enhance symptomatic Zika illness in dengue-seropositive individuals, rather it reduced the risk of VCZ. Zika infection boosted preexisting vaccine-induced or naturally occurring dengue-neutralizing antibodies.

Published

2020

17. Multidimensional analyses reveal modulation of adaptive and innate immune subsets by tuberculosis vaccines

Author

Ann M. Ginsberg, Thomas J. Scriba, Mark Hatherill, Carlos A. DiazGranados, William Fulp, Mzwandile Erasmus, Greg Finak, C Study Team, Hennie Geldenhuys, Sanjay Gurunathan, Asma Toefy, Munyaradzi Musvosvi, Linda-Gail Bekker, Muki Shey, Virginie Rozot, Nicole Bilek, David A. Hokey, Frances Rantangee, Lebohang Makhethe, Simbarashe Mabwe, and Elisa Nemes

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Protein vaccines, Adolescent, Live attenuated vaccines, Medicine (miscellaneous), Adaptive Immunity, Article, General Biochemistry, Genetics and Molecular Biology, Mycobacterium tuberculosis, Interferon-gamma, 03 medical and health sciences, 0302 clinical medicine, Immune system, Humans, Tuberculosis, Child, Tuberculosis Vaccines, lcsh:QH301-705.5, Tuberculosis, Pulmonary, Innate immune system, Attenuated vaccine, biology, Th1 Cells, biology.organism_classification, Immunity, Innate, In vitro, Vaccination, 030104 developmental biology, lcsh:Biology (General), Immunology, BCG Vaccine, Cytokines, Natural Killer T-Cells, Tumor necrosis factor alpha, Pathogens, General Agricultural and Biological Sciences, Tuberculosis vaccines, 030215 immunology

Abstract

We characterize the breadth, function and phenotype of innate and adaptive cellular responses in a prevention of Mycobacterium tuberculosis infection trial. Responses are measured by whole blood intracellular cytokine staining at baseline and 70 days after vaccination with H4:IC31 (subunit vaccine containing Ag85B and TB10.4), Bacille Calmette-Guerin (BCG, a live attenuated vaccine) or placebo (n = ~30 per group). H4:IC31 vaccination induces Ag85B and TB10.4-specific CD4 T cells, and an unexpected NKTlike subset, that expresses IFN-γ, TNF and/or IL-2. BCG revaccination increases frequencies of CD4 T cell subsets that either express Th1 cytokines or IL-22, and modestly increases IFNγ-producing NK cells. In vitro BCG re-stimulation also triggers responses by donor-unrestricted T cells, which may contribute to host responses against mycobacteria. BCG, which demonstrated efficacy against sustained Mycobacterium tuberculosis infection, modulates multiple immune cell subsets, in particular conventional Th1 and Th22 cells, which should be investigated in discovery studies of correlates of protection., Virginie Rozot and Elisa Nemes et al. report comprehensive profiling of immune responses from participants in a recent clinical trial of the H4:IC31 and BCG vaccines against Mycobacterium tuberculosis infection. Using a novel analysis platform, they uncover complex vaccine-induced modulation of different immune cell subsets.

Published

2020

18. Immune Response Persistence and Safety of a Booster Dose of the Tetravalent Dengue Vaccine in Adolescents and Adults Who Previously Completed the 3-dose Schedule 4-5 Years Earlier in Latin America: A Randomized Placebo-controlled Trial

Author

José Luis Arredondo-García, Doris Maribel Rivera, Ana Paula Perroud, Luis Andrey Rojas Peñalosa, Betzana Zambrano, Margarita Cortés, Gustavo H. Dayan, Fernando Noriega, Reynaldo Dietze, Carlos A. DiazGranados, Frédérique Jantet-Blaudez, Enid J Garcia-Rivera, Anke Pagnon, Hao Wang, Matthew Bonaparte, and Diana Coronel

Subjects

Microbiology (medical), Adult, Male, medicine.medical_specialty, Adolescent, Immunization, Secondary, Dengue Vaccines, Booster dose, Dengue virus, medicine.disease_cause, Placebo, Antibodies, Viral, complex mixtures, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Plaque reduction neutralization test, Neutralization Tests, 030225 pediatrics, Internal medicine, medicine, Humans, 030212 general & internal medicine, Vaccines, Combined, Neutralizing antibody, Child, Dengue vaccine, Immunization Schedule, Booster (rocketry), biology, business.industry, Dengue Virus, medicine.disease, Antibodies, Neutralizing, Infectious Diseases, Latin America, Pediatrics, Perinatology and Child Health, biology.protein, Female, business, Immunologic Memory, Follow-Up Studies

Abstract

Background We previously described an increased immune response 28 days after a booster dose of the live, attenuated, tetravalent dengue vaccine (CYD-TDV) in healthy adolescents and adults in Latin America (CYD64, NCT02623725). This follow-up study evaluated immune response persistence and safety of a CYD-TDV booster dose up to Month (M) 24 post-booster. Methods This study included 250 participants who previously received 3 primary doses of CYD-TDV in the CYD13 (NCT00993447) and CYD30 (NCT01187433) studies, and who were randomized 4-5 years later to receive a CYD-TDV booster or placebo (3:1). Dengue neutralizing antibodies against the parental dengue virus strains were assessed using the plaque reduction neutralization test (PRNT50) at M6, M12, and M24 post-booster. Post-booster memory B-cell responses were assessed in a subset of participants using the FluoroSpot assay up to M12 post-booster. Results In the CYD-TDV group (n = 187), dengue neutralizing antibody geometric mean titers (GMTs) declined from the peak at day 28 through to M24 for all serotypes. GMTs at M24 were similar to those at pre-booster among baseline dengue seropositives. A similar trend was observed for baseline dengue seronegatives, albeit at a lower magnitude. Previous vaccination-induced detectable B-cell memory responses in seropositives and seronegatives that decreased to pre-booster levels at M12 post-booster. The CYD-TDV booster dose was well-tolerated. Conclusions In baseline dengue seropositives, following a CYD-TDV booster dose administered 4-5 years after primary immunization, dengue neutralizing antibody GMTs and B-cell memory responses peaked in the short-term before gradually decreasing over time. A CYD-TDV booster dose could improve protection against dengue during outbreak periods.

Published

2020

19. Analysis of Hospitalized and Severe Dengue Cases Over the 6 years of Follow-up of the Tetravalent Dengue Vaccine (CYD-TDV) Efficacy Trials in Asia and Latin America

Author

Leilani Sanchez, Ana Paula Perroud, Gustavo H. Dayan, Tifany Machabert, Humberto Reynales, Betzana Zambrano, Claire Vigne, Stephen Savarino, Thelma Laot, Sri Rezeki Hadinegoro, Carlos A. DiazGranados, Owen Haney, Matthew Bonaparte, Alex Luedtke, Diana Coronel, Danaya Chansinghakul, Fernando Noriega, Yukun Wu, Alain Bouckenooghe, Maria Rosario Capeding, Brenda L. Price, Carina Frago, and Remi Forrat

Subjects

Microbiology (medical), medicine.medical_specialty, Asia, Dengue Vaccines, Placebo, Antibodies, Viral, Vaccines, Attenuated, Dengue fever, Internal medicine, Post-hoc analysis, Medicine, Humans, Severe Dengue, Vaccines, Combined, Child, Dengue vaccine, business.industry, Hazard ratio, serostatus, VCD, Dengue Virus, medicine.disease, dengue, Confidence interval, Clinical trial, Major Articles and Commentaries, Infectious Diseases, Latin America, AcademicSubjects/MED00290, CYD-TDV, business, Serostatus, Follow-Up Studies

Abstract

Background CYD-TDV, a live, attenuated, tetravalent dengue vaccine, has been approved for the prevention of symptomatic dengue in previously dengue exposed individuals. This post hoc analysis assessed hospitalized and severe virologically confirmed dengue (VCD) over the complete 6-year follow-up of 3 CYD-TDV efficacy studies (CYD14, CYD15, and CYD23/CYD57). Methods The main outcomes were hazard ratios (HRs) for hospitalized or severe VCD by baseline dengue serostatus, focusing on those who were seropositive, and by age at immunization (, The final completed 6-year follow-up of 3 CYD-TDV randomized trials in Asia and Latin America confirms the influence of age and prior dengue infection on vaccine effect, indicating protection against hospitalized and severe dengue in seropositives ≥6 years old.

Published

2020

20. Accuracy and efficacy of pre-dengue vaccination screening for previous dengue infection with five commercially available immunoassays: a retrospective analysis of phase 3 efficacy trials

Author

Matthew Bonaparte, Gustavo H. Dayan, Wang Hao, Carlos A. DiazGranados, Shekema Hodge, Yaniv Lustig, Eli Schwartz, Yasemin Ataman-Önal, Ming Zhu, Stephen Savarino, and Remi Forrat

Subjects

Male, medicine.medical_specialty, Adolescent, 030231 tropical medicine, Dengue Vaccines, Antibodies, Viral, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Neutralization Tests, Internal medicine, Retrospective analysis, medicine, Humans, Mass Screening, 030212 general & internal medicine, Igg elisa, Child, Dengue vaccine, Retrospective Studies, Immunoassay, medicine.diagnostic_test, business.industry, Patient Selection, Reproducibility of Results, Dengue Virus, Vaccine efficacy, medicine.disease, Vaccination, Infectious Diseases, Clinical Trials, Phase III as Topic, Child, Preschool, Female, Reagent Kits, Diagnostic, Serostatus, business

Abstract

Summary Background The tetravalent dengue vaccine (CYD-TDV) has been shown to provide protection against dengue disease over 5-year follow-up in participants with previous dengue infection, but increased the risk of dengue hospitalisation and severe dengue during long-term follow-up in those without previous dengue infection. WHO recommended pre-vaccination screening to identify those with previous dengue infection (ie, dengue seropositive) who would benefit from vaccination. We re-evaluated CYD-TDV efficacy in those identified as dengue seropositive using five commercially available immunoassays, and assessed immunoassay performance. Methods We included participants in the immunogenicity subsets of the phase 3 CYD14 ( NCT01373281 ) and CYD15 ( NCT01374516 ) CYD-TDV efficacy trials, which enrolled children aged 2–16 years in 2011–12 in five countries in the Asia-Pacific region (CYD14) and five Latin American countries (CYD15). Participants assessed had received at least one injection of study drug (CYD-TDV or placebo) and had baseline samples available. We tested baseline samples by IgG-based immunoassays to classify baseline dengue serostatus, using two ELISAs (EUROIMMUN and Panbio) and three rapid diagnostic tests (RDTs; TELL ME FAST, SD BIOLINE, and OnSite). Vaccine efficacy in preventing symptomatic, hospitalised, and severe virologically confirmed dengue was determined for participants who tested positive by each immunoassay. The specificity and sensitivity of each immunoassay was determined as percentage negative and positive agreement compared with the reference algorithm, which used dengue plaque reduction neutralisation test with 50% and 90% cutoffs and non-structural protein 1 IgG ELISA results to assign baseline serostatus. Findings Samples were available for 3967 participants, 2735 (69·0%) of whom were classified as seropositive by the reference algorithm. Vaccine efficacy against symptomatic virologically confirmed dengue in immunoassay-positive participants was high across all five immunoassays (EUROIMMUN ELISA 88·2% [95% CI 77·3 to 93·9], Panbio ELISA 87·6% [76·7 to 93·4], TELL ME FAST RDT 88·8% [67·0 to 96·2], SD BIOLINE RDT 82·8% [66·9 to 91·1], and OnSite RDT 89·7% [64·6 to 97·0]), as was vaccine efficacy against hospitalised virologically confirmed dengue (EUROIMMUN-ELISA 72·8% [38·9 to 87·9], Panbio ELISA 77·5% [52·8 to 89·3], TELL ME FAST RDT 92·4% [37·8 to 99·1], SD BIOLINE RDT 87·2% [54·5 to 96·4], and OnSite RDT 73·7% [–5·1 to 93·4]) and severe virologically confirmed dengue (EUROIMMUN ELISA 86·9% [–16·8 to 98·5], Panbio ELISA 91·3% [27·6 to 99·0], TELL ME FAST RDT 100·0% [not estimable to 100·0%], SD BIOLINE RDT 89·4% [9·6 to 98·8], and OnSite RDT 73·4% [–193·7 to 97·6]). The immunoassays exhibited high specificity (≥98·8% for all immunoassays apart from SD BIOLINE RDT) but variable sensitivities, with higher sensitivities observed for the ELISAs (EUROIMMUN 89·2% [87·9 to 90·3] and Panbio 92·5 [91·4 to 93·5]) than the RDTs (TELL ME FAST 52·5% [50·6 to 54·4], SD BIOLINE 71·1% [69·3 to 72·8], and OnSite 47·6% [45·7 to 49·5]). Interpretation Our findings suggest that these immunoassays could be used for pre-vaccination screening for CYD-TDV as tools to assist risk stratification until more sensitive and convenient tests become available. Funding Sanofi Pasteur.

Published

2020

21. Efficacy after 1 and 2 doses of CYD-TDV in dengue endemic areas by dengue serostatus

Author

Fernando Noriega, Stephen Savarino, Gustavo H. Dayan, Tifany Machabert, Alain Bouckenooghe, Edith Langevin, Betzana Zambrano, Remi Forrat, Carina Frago, and Carlos A. DiazGranados

Subjects

medicine.medical_specialty, 030231 tropical medicine, Dengue Vaccines, Antibodies, Viral, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Plaque reduction neutralization test, Internal medicine, medicine, Humans, 030212 general & internal medicine, Neutralizing antibody, Dengue vaccine, Aged, General Veterinary, General Immunology and Microbiology, biology, business.industry, Public Health, Environmental and Occupational Health, Dengue Virus, Vaccine efficacy, medicine.disease, Antibodies, Neutralizing, Titer, Regimen, Infectious Diseases, biology.protein, Molecular Medicine, business, Serostatus

Abstract

A simplified dose regimen of the live, attenuated, tetravalent dengue vaccine (CYD-TDV) could have the potential to facilitate easier implementation of immunization programs against symptomatic virologically-confirmed dengue (VCD) in dengue seropositive individuals aged ≥ 9 years. This post-hoc analysis of two Phase III studies (CYD14 [NCT01373281] and CYD15 [NCT01374516]) in dengue endemic areas assessed the efficacy of CYD-TDV by dengue serostatus between dose 1 and 2 (at Month [M] 6), between dose 2 and 3 (at M12), and from dose 3 to M25. Baseline dengue serostatus (seropositive or seronegative) was determined based on measured dengue neutralizing antibody titers with the 50% plaque reduction neutralization test (PRNT50) or ascertained by logistic regression-based multiple imputation (MI) to predict PRNT50. Vaccine efficacy against symptomatic VCD was assessed by age and baseline dengue serostatus using a case-cohort framework. Dengue neutralizing antibody geometric mean titers (GMTs) were measured with the PRNT50 at 28 days post-dose 2 and 3. Vaccine efficacy estimates in seropositive participants aged ≥ 9 years at post-dose 1, 2, and 3 were 80.5% (95% CI, 66.2, 88.7), 82.0% (95% CI, 70.5, 89.0), and 75.2% (95% CI, 65.9, 81.9), respectively. In seropositive participants aged

Published

2020

22. A phase 1b randomized study of the safety and immunological responses to vaccination with H4:IC31, H56:IC31, and BCG revaccination in Mycobacterium tuberculosis-uninfected adolescents in Cape Town, South Africa

Author

Anthony Williams, Georgia D. Tomaras, Andrew Fiore-Gartland, One B. Dintwe, Kathryn Tucker Rutkowski, Aeras A Protocol Team, Peter Andersen, Keren Middelkoop, Hvtn, Kelly E. Seaton, M. Juliana McElrath, Linda-Gail Bekker, Erica Andersen-Nissen, James G. Kublin, Ann M. Ginsberg, Dereck Tait, Stephen C. De Rosa, Ingrid Kromann, Julia Hutter, Carlos A. DiazGranados, April K. Randhawa, Morten Ruhwald, and Maurine D. Miner

Subjects

Research paper, Tuberculosis, 01 natural sciences, QuantiFERON, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Antigen, Medicine, BCG, 030212 general & internal medicine, H56:IC31, 0101 mathematics, lcsh:R5-920, biology, business.industry, Immunogenicity, 010102 general mathematics, General Medicine, Vaccine efficacy, medicine.disease, biology.organism_classification, Vaccination, Immunology, biology.protein, Antibody, business, lcsh:Medicine (General), H4:IC31

Abstract

Background: Tuberculosis (TB) remains the leading cause of infectious disease-related death. Recently, a trial of BCG revaccination and vaccination with H4:IC31, a recombinant protein vaccine, in South African adolescents (Aeras C-040-404) showed efficacy in preventing sustained QuantiFERON (QFT) conversion, a proxy for Mycobacterium tuberculosis (M.tb) infection. A phase 1b trial of 84 South African adolescents was conducted, concurrent with Aeras C-040-404, to assess the safety and immunogenicity of H4:IC31, H56:IC31 and BCG revaccination, and to identify and optimize immune assays for identification of candidate correlates of protection in efficacy trials. Methods: Two doses of H4:IC31 and H56:IC31 vaccines were administered intramuscularly (IM) 56 days apart, and a single dose of BCG (2–8 × 105 CFU) was administered intradermally (ID). T-cell and antibody responses were measured using intracellular cytokine staining and binding antibody assays, respectively. Binding antibodies and CD4+/CD8+ T-cell responses to H4- and H56-matched antigens were measured in samples from all participants. The study was designed to characterize safety and immunogenicity and was not powered for group comparisons. (Clinicaltrials.gov NCT02378207). Findings: In total, 481 adolescents (mean age 13·9 years) were screened; 84 were enrolled (54% female). The vaccines were generally safe and well-tolerated, with no reported severe adverse events related to the study vaccines. H4:IC31 and H56:IC31 elicited CD4+ T cells recognizing vaccine-matched antigens and H4- and H56-specific IgG binding antibodies. The highest vaccine-induced CD4+ T-cell response rates were for those recognizing Ag85B in the H4:IC31 and H56:IC31 vaccinated groups. BCG revaccination elicited robust, polyfunctional BCG-specific CD4+ T cells, with no increase in H4- or H56-specific IgG binding antibodies. There were few antigen-specific CD8+ T-cell responses detected in any group. Interpretation: BCG revaccination administered as a single dose ID and both H4:IC31 and H56:IC31 administered as 2 doses IM had acceptable safety profiles in healthy, QFT-negative, previously BCG-vaccinated adolescents. Characterization of the assays and the immunogenicity of these vaccines may help to identify valuable markers of protection for upcoming immune correlates analyses of C-040-404 and future TB vaccine efficacy trials. Funding: NIAID and Aeras. Keywords: Mycobacterium tuberculosis, H4:IC31, H56:IC31, BCG

Published

2020

23. Late Boosting of the RV144 Regimen with AIDSVAX B/E and ALVAC-HIV in HIV-Uninfected Thai Volunteers, a Randomised Controlled Trial

Author

Piyathida Sroysuwan, Natthapol Kosashunhanan, Sebastian Molnar, Jerome H. Kim, Alexandra Schuetz, Taweewat Supindham, Elizabeth Heger, Sandhya Vasan, Phiromrat Rakyat, Suwat Chariyalertsak, Nittaya Phanuphak, Siriluck Teerachia, Suchada Chinaworapong, Nongluck Sangnoi, Oranitcha Kaewthip, Sorachai Nitayaphan, Surat Jongrakthaitae, Pornchanok Panjapornsuk, Michael A. Eller, Puttachard Saengtawan, Weerawan Chuenarom, Nuntisa Chotirosniramit, Pornsuk V. Grandin, Sirinan Madnote, Benjaluck Phonrat, Rungsun Rerknimitr, Narongrid Sirisopana, Lindsay Wieczorek, Siriwat Akapirat, Chirapa Eamsila, Faruk Sinangil, Kirsten Smith, James Tartaglia, Poonam Pegu, Dohoon Kim, Carter Lee, Peter Dawson, Saowanit Getchalarat, Robert J. O'Connell, Nicos Karasavvas, Jiraporn Puangkaew, Patcharaphan Sugandhavesa, Nitiya Chomchey, Punnee Pitisuttithum, Jean-Louis Excler, Boonlure Pruenglampoo, Yingjun Zhou, Yupa Sabmee, Jittima Dhitavat, Merlin L. Robb, Jesse Schoen, Victoria R. Polonis, Nelson L. Michael, Boot Kaewboon, Nipat Teeratakulpisarn, Bessara Nuntapinit, Wanlaya Labwech, Eugene Kroon, Viseth Ngauy, Prapaporn Savaraj, Jaranit Kaewkungwal, Pawinee Jarujareet, Nampueng Churikanont, Surawach Rittiroongrad, Somsak Chantakulkij, Anant Phramtong, Rapee Trichavaroj, Carlos A. DiazGranados, Silvia Ratto-Kim, Sanjay Phogat, Mark de Souza, Arom Pitisuthitham, and Nipattra Tragonlugsana

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Epidemiology, Immunology, Immunization, Secondary, HIV Infections, Placebo, Article, law.invention, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Randomized controlled trial, Double-Blind Method, law, Virology, Internal medicine, Medicine, Humans, 030212 general & internal medicine, AIDS Vaccines, Reactogenicity, business.industry, Vaccine trial, HIV, Thailand, 030112 virology, Vaccination, Clinical trial, Regimen, Infectious Diseases, AIDSVAX, Female, business

Abstract

BACKGROUND: The RV144 phase 3 vaccine trial in Thailand demonstrated that ALVAC-HIV (vCP1521) and AIDSVAX® B/E administration over six months resulted in a 31% efficacy in preventing HIV acquisition. In this trial, we assessed the immunologic impact of an additional vaccine boost to the RV144 regimen at varying intervals between the priming vaccine series and the boost. METHODS: RV306 is a double-blind, placebo-controlled, randomized clinical trial conducted in three clinical sites in Thailand. HIV-uninfected volunteers aged 20–40 randomly received the primary RV144 vaccine series at months 0, 1, 3, and 6, with no additional boost (Group I), additional AIDSVAX® B/E and ALVAC-HIV (vcp1521) at month 12 (Group II), AIDSVAX® B/E alone at month 12 (Group III), AIDSVAX® B/E and ALVAC-HIV at month 15 or 18 (Groups IVa or IVb), or placebo and were followed for 24 months. A randomization schedule was centrally generated with fixed sized strata for RIHES Chiang Mai (n=60) and combined Bangkok clinics (n=300). Primary outcomes were to assess the safety and tolerability of these vaccination regimens and characterize and compare cellular and humoral immune responses between the RV144 series alone and late boosts at different timepoints. Safety and tolerability outcomes were assessed by evaluating local and systemic reactogenicity and adverse events in all participants. Primary immunogenicity outcomes were evaluated by comparing peak humoral responses (HIV-specific IgG and IgA ELISA) and cellular responses (HIV-specific intracellular cytokine staining and polyfunctionality) two weeks post final vaccination among per-protocol participants who completed all vaccinations. This trial is registered at (ClinicalTrials.gov (NCT01931358); clinical follow up is now complete. FINDINGS: Between 28 October 2013 and 29 April 2014, 367 participants were enrolled, of whom 27 were assigned active vaccination in Group I, 102 in Group II, 101 in Group III, 52 in Group IVa, 51 in Group IVb, and 34 combined placebo across all groups. Late boosting did not induce vaccine-related serious adverse events. There were no significant differences in the occurrence or severity of local or systemic reactogenicity across active groups. Groups with late boosts (Groups II, III, IVa, and IVb) had increased peak plasma IgG binding antibody levels against gp70 V1V2 relative to Group I vaccine recipients with no late boost (gp70V1V2 92TH023 adjusted p < 0·02 for each; gp70V1V2 Case A2 adjusted p month 15 (Group IVa) > month 12 (Groups II+III) > no late boost (Group I). Groups with late boosts had increased both functionality and polyfunctionality scores relative to vaccine recipients with no late boost (all adjusted p < 0·05, except for polyfunctionality score in Group I vs in Group IVb p < 0·01). INTERPRETATION: Taken together, these results suggest that additional boosting of the RV144 regimen with longer intervals between the primary vaccination series and late boost improved immune responses and may improve the efficacy of preventing HIV acquisition. FUNDING: US National Institute of Allergy and Infectious Diseases (NIAID) and U.S. Department of the Army.

Published

2020

24. Safety and immune responses after a 12-month booster in healthy HIV-uninfected adults in HVTN 100 in South Africa: A randomized double-blind placebo-controlled trial of ALVAC-HIV (vCP2438) and bivalent subtype C gp120/MF59 vaccines

Author

Kathryn Therese. Mngadi, Vijay L. Mehra, Kristen W. Cohen, Glenda Gray, Shannon Grant, Zoe Moodie, Brodie Daniels, Marguerite Koutsoukos, Sanjay Phogat, Peter B. Gilbert, M. Juliana McElrath, Nonhlanhla N. Mkhize, Chenchen Yu, Georgia D. Tomaras, Olivier Van Der Meeren, Linda-Gail Bekker, James G. Kublin, Nicole Frahm, Carlos A. DiazGranados, Mary Allen, Lawrence Corey, Fatima Laher, Carter Bentley, Mookho Malahleha, Michael Pensiero, Lynn Morris, Kevin O. Saunders, Nicole L. Yates, Nicole Grunenberg, David C. Montefiori, and Craig Innes

Subjects

CD4-Positive T-Lymphocytes, Male, Physiology, Human Immunodeficiency Virus Proteins, Placebo-controlled study, Antibody Response, HIV Infections, 030204 cardiovascular system & hematology, Gastroenterology, Biochemistry, Memory T cells, law.invention, White Blood Cells, South Africa, 0302 clinical medicine, Immunogenicity, Vaccine, Randomized controlled trial, law, Animal Cells, Immune Physiology, Medicine and Health Sciences, Public and Occupational Health, 030212 general & internal medicine, Booster Doses, Immune Response, Not evaluated, AIDS Vaccines, Vaccines, Immune System Proteins, T Cells, Headache, General Medicine, Vaccination and Immunization, Arthralgia, 3. Good health, Vaccination, Infectious Diseases, Medicine, Female, Cellular Types, Research Article, Adult, medicine.medical_specialty, Infectious Disease Control, Immune Cells, Immunology, Immunization, Secondary, Placebo, Injections, Intramuscular, Antibodies, 03 medical and health sciences, Young Adult, Double-Blind Method, Internal medicine, Injection site reaction, medicine, Humans, Adverse effect, Blood Cells, business.industry, Biology and Life Sciences, Proteins, Cell Biology, medicine.disease, Antibodies, Neutralizing, Injection Site Reaction, Regimen, Immunoglobulin G, Preventive Medicine, business

Abstract

Background HVTN 100 evaluated the safety and immunogenicity of an HIV subtype C pox-protein vaccine regimen, investigating a 12-month booster to extend vaccine-induced immune responses. Methods and findings A phase 1–2 randomized double-blind placebo-controlled trial enrolled 252 participants (210 vaccine/42 placebo; median age 23 years; 43% female) between 9 February 2015 and 26 May 2015. Vaccine recipients received ALVAC-HIV (vCP2438) alone at months 0 and 1 and with bivalent subtype C gp120/MF59 at months 3, 6, and 12. Antibody (IgG, IgG3 binding, and neutralizing) and CD4+ T-cell (expressing interferon-gamma, interleukin-2, and CD40 ligand) responses were evaluated at month 6.5 for all participants and at months 12, 12.5, and 18 for a randomly selected subset. The primary analysis compared IgG binding antibody (bAb) responses and CD4+ T-cell responses to 3 vaccine-matched antigens at peak (month 6.5 versus 12.5) and durability (month 12 versus 18) timepoints; IgG responses to CaseA2_gp70_V1V2.B, a primary correlate of risk in RV144, were also compared at these same timepoints. Secondary and exploratory analyses compared IgG3 bAb responses, IgG bAb breadth scores, neutralizing antibody (nAb) responses, antibody-dependent cellular phagocytosis, CD4+ polyfunctionality responses, and CD4+ memory sub-population responses at the same timepoints. Vaccines were generally safe and well tolerated. During the study, there were 2 deaths (both in the vaccine group and both unrelated to study products). Ten participants became HIV-infected during the trial, 7% (3/42) of placebo recipients and 3% (7/210) of vaccine recipients. All 8 serious adverse events were unrelated to study products. Less waning of immune responses was seen after the fifth vaccination than after the fourth, with higher antibody and cellular response rates at month 18 than at month 12: IgG bAb response rates to 1086.C V1V2, 21.0% versus 9.7% (difference = 11.3%, 95% CI = 0.6%–22.0%, P = 0.039), and ZM96.C V1V2, 21.0% versus 6.5% (difference = 14.5%, 95% CI = 4.1%–24.9%, P = 0.004). IgG bAb response rates to all 4 primary V1V2 antigens were higher 2 weeks after the fifth vaccination than 2 weeks after the fourth vaccination: 87.7% versus 75.4% (difference = 12.3%, 95% CI = 1.7%–22.9%, P = 0.022) for 1086.C V1V2, 86.0% versus 63.2% (difference = 22.8%, 95% CI = 9.1%–36.5%, P = 0.001) for TV1c8.2.C V1V2, 67.7% versus 44.6% (difference = 23.1%, 95% CI = 10.4%–35.7%, P < 0.001) for ZM96.C V1V2, and 81.5% versus 60.0% (difference = 21.5%, 95% CI = 7.6%–35.5%, P = 0.002) for CaseA2_gp70_V1V2.B. IgG bAb response rates to the 3 primary vaccine-matched gp120 antigens were all above 90% at both peak timepoints, with no significant differences seen, except a higher response rate to ZM96.C gp120 at month 18 versus month 12: 64.5% versus 1.6% (difference = 62.9%, 95% CI = 49.3%–76.5%, P < 0.001). CD4+ T-cell response rates were higher at month 18 than month 12 for all 3 primary vaccine-matched antigens: 47.3% versus 29.1% (difference = 18.2%, 95% CI = 2.9%–33.4%, P = 0.021) for 1086.C, 61.8% versus 38.2% (difference = 23.6%, 95% CI = 9.5%–37.8%, P = 0.001) for TV1.C, and 63.6% versus 41.8% (difference = 21.8%, 95% CI = 5.1%–38.5%, P = 0.007) for ZM96.C, with no significant differences seen at the peak timepoints. Limitations were that higher doses of gp120 were not evaluated, this study was not designed to investigate HIV prevention efficacy, and the clinical significance of the observed immunological effects is uncertain. Conclusions In this study, a 12-month booster of subtype C pox-protein vaccines restored immune responses, and slowed response decay compared to the 6-month vaccination. Trial registration ClinicalTrials.gov NCT02404311. South African National Clinical Trials Registry (SANCTR number: DOH--27-0215-4796)., Fatima Laher and co-authors report on safety and immune responses in a randomized trial of a candidate HIV vaccine incorporating a "booster" vaccination., Author summary Why was this study done? The RV144 vaccine trial, which tested a pox-protein regimen designed against HIV subtypes B and E, showed modest efficacy in preventing HIV acquisition. However, efficacy and vaccine-induced immune responses declined considerably after the first year. Our clinical trial, HVTN 100, investigated whether adding a booster at month 12 to a similar vaccine regimen, tailored against subtype C HIV, would prolong immune responses, and also evaluated its safety. What did the researchers do and find? We gave intramuscular injections of ALVAC-HIV (vCP2438) alone at months 0 and 1 and with bivalent subtype C gp120/MF59 at months 3, 6, and 12 to 210 vaccine recipients. We administered placebo to 42 participants. We tested antibody (IgG, IgG3 binding, antibody-dependent cellular phagocytosis, and neutralizing) and cellular (T cells expressing interferon-gamma, interleukin-2, or CD40 ligand) immune responses at month 6.5 in all participants and at months 12, 12.5, and 18 in a randomly chosen subset. We evaluated safety for 18 months. Vaccines were generally safe and well tolerated. Antibody and cellular response rates were higher after the 12-month booster than after the 6-month vaccination. What do these findings mean? Adding a booster osf subtype C pox-protein vaccines at month 12 can improve the durability of vaccine-induced immune responses. The ongoing phase 2b–3 trial HVTN 702 was designed to evaluate the efficacy of this regimen with month 12 and month 18 boosters.

Published

2020

25. Assessment of the long-term efficacy of a dengue vaccine against symptomatic, virologically-confirmed dengue disease by baseline dengue serostatus

Author

Alain Bouckenooghe, Carina Frago, Brenda L. Price, Margarita Cortés, Remi Forrat, Yukun Wu, Fernando Noriega, Zoe Moodie, Peter B. Gilbert, Carlos A. DiazGranados, Gustavo H. Dayan, and Edith Langevin

Subjects

Pediatrics, medicine.medical_specialty, Asia, 030231 tropical medicine, Dengue Vaccines, Antibodies, Viral, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Asia pacific, Medicine, Humans, 030212 general & internal medicine, Child, Dengue vaccine, General Veterinary, General Immunology and Microbiology, business.industry, Public Health, Environmental and Occupational Health, Expansion phase, Dengue Virus, medicine.disease, Vaccine efficacy, Infectious Diseases, Latin America, Molecular Medicine, business, Serostatus, Dengue disease

Abstract

CYD-TDV is a live, attenuated, tetravalent dengue vaccine licensed in 21 countries. We undertook a post-hoc analysis of the long-term efficacy of CYD-TDV during the surveillance expansion phase (SEP) of two Phase III studies (CYD14 in the Asia-Pacific region; CYD15 in Latin America). The SEP included approximately Year 5 and the entire Year 6 of follow-up after the first study injection. Vaccine efficacy against symptomatic virologically-confirmed dengue (VCD) was assessed by participant age (any age, ≥9,9, 2-5, and 6-8 years at the time of the first injection) and baseline dengue serostatus using a case-cohort framework. Baseline dengue serostatus was estimated by several methods including logistic regression-based multiple imputation (MI) to predict PRNT

Published

2019

26. Effect of Dengue Serostatus on Dengue Vaccine Safety and Efficacy

Author

Fernando Noriega, Tifany Machabert, Ted Westling, Margarita Cortés, Alena Khromava, Danaya Chansinghakul, Betzana Zambrano, Ming Zhu, Josh Chen, Matthew Bonaparte, Alex Luedtke, Edith Langevin, Saranya Sridhar, Alain Bouckenooghe, Carina Frago, Su-Peing Ng, Zoe Moodie, Sanjay Gurunathan, Cesar Mascareñas, Stephen Savarino, Peter B. Gilbert, Carlos A. DiazGranados, and Annick Moureau

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Dengue Vaccines, Enzyme-Linked Immunosorbent Assay, Viral Nonstructural Proteins, Antibodies, Viral, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Neutralization test, Post-hoc analysis, Humans, Medicine, 030212 general & internal medicine, Imputation (statistics), Child, Dengue vaccine, Proportional Hazards Models, business.industry, Proportional hazards model, Case-control study, General Medicine, Dengue Virus, medicine.disease, Hospitalization, Treatment Outcome, 030104 developmental biology, Case-Control Studies, Child, Preschool, Female, business, Serostatus

Abstract

In efficacy trials of a tetravalent dengue vaccine (CYD-TDV), excess hospitalizations for dengue were observed among vaccine recipients 2 to 5 years of age. Precise risk estimates according to observed dengue serostatus could not be ascertained because of the limited numbers of samples collected at baseline. We developed a dengue anti-nonstructural protein 1 (NS1) IgG enzyme-linked immunosorbent assay and used samples from month 13 to infer serostatus for a post hoc analysis of safety and efficacy.In a case-cohort study, we reanalyzed data from three efficacy trials. For the principal analyses, we used baseline serostatus determined on the basis of measured (when baseline values were available) or imputed (when baseline values were missing) titers from a 50% plaque-reduction neutralization test (PRNTAmong dengue-seronegative participants 2 to 16 years of age, the cumulative 5-year incidence of hospitalization for VCD was 3.06% among vaccine recipients and 1.87% among controls, with a hazard ratio (vaccine vs. control) through data cutoff of 1.75 (95% confidence interval [CI], 1.14 to 2.70). Among dengue-seronegative participants 9 to 16 years of age, the cumulative incidence of hospitalization for VCD was 1.57% among vaccine recipients and 1.09% among controls, with a hazard ratio of 1.41 (95% CI, 0.74 to 2.68). Similar trends toward a higher risk among seronegative vaccine recipients than among seronegative controls were also found for severe VCD. Among dengue-seropositive participants 2 to 16 years of age and those 9 to 16 years of age, the cumulative incidence of hospitalization for VCD was 0.75% and 0.38%, respectively, among vaccine recipients and 2.47% and 1.88% among controls, with hazard ratios of 0.32 (95% CI, 0.23 to 0.45) and 0.21 (95% CI, 0.14 to 0.31). The risk of severe VCD was also lower among seropositive vaccine recipients than among seropositive controls.CYD-TDV protected against severe VCD and hospitalization for VCD for 5 years in persons who had exposure to dengue before vaccination, and there was evidence of a higher risk of these outcomes in vaccinated persons who had not been exposed to dengue. (Funded by Sanofi Pasteur; ClinicalTrials.gov numbers, NCT00842530 , NCT01983553 , NCT01373281 , and NCT01374516 .).

Published

2018

27. Accuracy, efficacy and safety of dengue CYD-TDV pre-vaccination screening with 5 existing IgG serotests: Retrospective analysis of phase III trials

Author

Y. Ataman-Onal, R. Forrat, H. Wang, Yaniv Lustig, S. Hodge, Eli Schwartz, Ming Zhu, G. Dayan, Carlos A. DiazGranados, Matthew Bonaparte, and Stephen Savarino

Subjects

Microbiology (medical), medicine.medical_specialty, Phase iii trials, business.industry, General Medicine, medicine.disease, lcsh:Infectious and parasitic diseases, Dengue fever, Vaccination, Infectious Diseases, Internal medicine, medicine, Retrospective analysis, lcsh:RC109-216, business

Published

2020

28. Randomized, Double-Blind Evaluation of Late Boost Strategies for HIV-Uninfected Vaccine Recipients in the RV144 HIV Vaccine Efficacy Trial

Author

Jaranit Kaewkungwal, Saintedym Wills, Carlos A. DiazGranados, Merlin L. Robb, Poonam Pegu, James Tartaglia, Rv Study Team, Allan C. deCamp, Nakorn Premsri, Alexandra Schuetz, Sanjay Garunathan, Michael A. Eller, Robert J. O'Connell, Nicos Karasavvas, Nathan Vandergrift, Sorachai Nitayaphan, Faruk Sinangil, Jean-Louis Excler, Punnee Pitisuttithum, Chitraporn Karnasuta, Nelson L. Michael, Silvia Ratto-Kim, Georgia D. Tomaras, Sanjay Phogat, Jerome H. Kim, Supachai Rerks-Ngarm, Sheetal Sawant, David C. Montefiori, Prayura Kunasol, Viseth Ngauy, Sandhya Vasan, and Peter Dawson

Subjects

Adult, Male, 0301 basic medicine, Immunization, Secondary, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Placebo, Immunoglobulin G, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Major Article, Humans, Immunology and Allergy, Medicine, 030212 general & internal medicine, HIV vaccine, Neutralizing antibody, AIDS Vaccines, biology, business.industry, Immunogenicity, Thailand, Antibodies, Neutralizing, Healthy Volunteers, Immunity, Humoral, Immunoglobulin A, Vaccination, 030104 developmental biology, Infectious Diseases, AIDSVAX, Immunology, HIV-1, biology.protein, Cytokines, Female, Antibody, business

Abstract

Background The RV144 ALVAC-HIV prime, AIDSVAX B/E boost afforded 60% efficacy against human immunodeficiency virus (HIV) acquisition at 1 year, waning to 31.2% after 3.5 years. We hypothesized that additional vaccinations might augment immune correlates of protection. Methods In a randomized placebo-controlled double-blind study of 162 HIV-negative RV144 vaccine recipients, we evaluated 2 additional boosts, given 6-8 years since RV144 vaccination, for safety and immunogenicity, at weeks 0 and 24. Study groups 1-3 received ALVAC-HIV+AIDSVAX B/E, AIDSVAX B/E, and ALVAC-HIV, respectively, or placebo. Results Vaccines were well tolerated. For groups 1 and 2, plasma immunoglobulin (Ig) G, IgA, and neutralizing antibody responses at week 2 were all significantly higher than 2 weeks after the last RV144 vaccination. IgG titers against glycoprotein (gp) 70V1V2 92TH023 increased 14-fold compared with 2 weeks after the last RV144 vaccination (14069 vs 999; P < .001). Groups 1 and 2 did not differ significantly from each other, whereas group 3 was similar to placebo recipients. Responses in groups 1 and 2 declined by week 24 but were boosted by the second vaccination, albeit at lower magnitude than for week 2. Conclusions In RV144 vaccinees, AIDSVAX B/E with or without ALVAC-HIV 6-8 years after initial vaccination generated higher humoral responses than after RV144, but these responses were short-lived, and their magnitude did not increase with subsequent boost. Clinical Trials Registration NCT01435135.

Published

2017

29. Immune correlates of the Thai RV144 HIV vaccine regimen in South Africa

Author

Erica Andersen-Nissen, Nicole L. Yates, Erica Lazarus, Surita Roux, Peter B. Gilbert, Xiaoying Shen, John Hural, Linda-Gail Bekker, Craig Innes, Carlos A. DiazGranados, Nonhlanhla N. Mkhize, Fatima Laher, Nelson L. Michael, Edith Swann, M. Juliana McElrath, Georgia D. Tomaras, Abby Isaacs, Stephen C. De Rosa, Carter Lee, Ying Huang, Nicole Grunenberg, Lawrence Corey, Sanjay Phogat, Britta Flach, Glenda Gray, Lynn Morris, Guido Ferrari, Ryan L. Jensen, Faruk Sinangil, Sheetal Sawant, David C. Montefiori, James G. Kublin, April K. Randhawa, and Merlin L. Robb

Subjects

Adult, Male, 0301 basic medicine, HIV Antigens, T-Lymphocytes, T cell, CD40 Ligand, HIV Antibodies, Article, Immunoglobulin G, Placebos, Interferon-gamma, South Africa, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immune system, Phagocytosis, Antigen, Neutralization Tests, medicine, Humans, 030212 general & internal medicine, HIV vaccine, AIDS Vaccines, Antibody-dependent cell-mediated cytotoxicity, Principal Component Analysis, biology, business.industry, Immunogenicity, Vaccination, Antibody-Dependent Cell Cytotoxicity, virus diseases, General Medicine, Thailand, Immunity, Humoral, 030104 developmental biology, medicine.anatomical_structure, Antibody Formation, Immunology, biology.protein, Interleukin-2, Female, business

Abstract

One of the most successful HIV vaccines to date, the RV144 vaccine tested in Thailand, demonstrated correlates of protection including cross-clade V1V2 immunoglobulin G (IgG) breadth, Env-specific CD4+ T cell polyfunctionality, and antibody-dependent cellular cytotoxicity (ADCC) in vaccinees with low IgA binding. The HIV Vaccine Trials Network (HVTN) 097 trial evaluated this vaccine regimen in South Africa, where clade C HIV-1 predominates. We compared cellular and humoral responses at peak and durability immunogenicity time points in HVTN 097 and RV144 vaccinee samples, and evaluated vaccine-matched and cross-clade immune responses. At peak immunogenicity, HVTN 097 vaccinees exhibited significantly higher cellular and humoral immune responses than RV144 vaccinees. CD4+ T cell responses were more frequent in HVTN 097 irrespective of age and sex, and CD4+ T cell Env-specific functionality scores were higher in HVTN 097. Env-specific CD40L+ CD4+ T cells were more common in HVTN 097, with individuals having this pattern of expression demonstrating higher median antibody responses to HIV-1 Env. IgG and IgG3 binding antibody rates and response magnitude to gp120 vaccine- and V1V2 vaccine-matched antigens were higher or comparable in HVTN 097 than in RV144 ADCC, and ADCP functional antibody responses were elicited in HVTN 097. Env-specific IgG and CD4+ Env responses declined significantly over time in both trials. Overall, cross-clade immune responses associated with protection were better than expected in South Africa, suggesting wider applicability of this regimen.

Published

2019

30. Evaluation of rapid diagnostic tests and conventional enzyme-linked immunosorbent assays to determine prior dengue infection

Author

Bruno Guy, Eli Schwartz, Yasemin Ataman-Önal, Carlos A. DiazGranados, Stephen Savarino, Matthew Bonaparte, Sanjay Garg, Yaniv Lustig, and Lingyi Zheng

Subjects

Adult, Male, Adolescent, Point-of-Care Systems, 030231 tropical medicine, Enzyme-Linked Immunosorbent Assay, Antibodies, Viral, Sensitivity and Specificity, Dengue fever, Dengue, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Plaque reduction neutralization test, Neutralization Tests, Medicine, Humans, 030212 general & internal medicine, Child, Dengue vaccine, biology, business.industry, Yellow fever, Diagnostic test, General Medicine, Japanese encephalitis, Dengue Virus, Middle Aged, biology.organism_classification, medicine.disease, Serum samples, Virology, Flavivirus, Child, Preschool, Immunoglobulin G, Female, business

Abstract

Background In September 2018, the World Health Organization recommended that prevaccination screening be used with the tetravalent dengue vaccine (CYD-TDV), to ensure that only individuals with evidence of prior dengue infection (PDI) are vaccinated. Dengue rapid diagnostic tests (RDTs) would offer a potential solution for prevaccination screening at the point-of-care, but data on performance of available RDTs for identifying PDI are limited. We determined the suitability of four dengue RDTs and two conventional enzyme-linked immunosorbent assays (ELISAs) to identify PDI and evaluated cross-reactivity with co-circulating flaviviruses. Methods: Specificity was assessed using 534 dengue-negative [determined by 50% plaque reduction neutralization test (PRNT50)] serum samples from USA (n = 229) and dengue-endemic regions (n = 305). Sensitivity was assessed using 270 samples from recent (n = 90) or remote (n = 90) virologically confirmed prior dengue cases, and dengue PRNT50-positive samples (n = 90). Cross-reactivity was assessed in dengue-seronegative samples that were seropositive for yellow fever (n = 57), Japanese encephalitis (n = 37), West Nile (n = 59) or Zika (n = 41). Results: Dengue IgG RDTs and the Panbio ELISA exhibited favourable specificities (99–100%), higher than the Focus ELISA (95%). The RDTs had variable sensitivities (40–70%) that were lower than those of the ELISAs (≥90%). Cross-reactivity to other flaviviruses was low with RDTs (≤7%), but more significant with ELISAs (up to 51% for West Nile and 34% for Zika). No cross-reactivity to any of the four closely related flaviviruses was observed with the CTK Biotech RDT. For each SeroTest, sensitivity appeared similar in samples from individuals with recent ( Conclusions: In general, dengue IgG RDTs were found to be more specific and less cross-reactive than the ELISAs, but the latter were more sensitive for identifying PDI cases. Currently available RDTs could be temporizing tools for rapid and safe prevaccination screening until improved RDTs with increased sensitivity become available.

Published

2019

31. Late Boosting of the RV144 Regimen Improves the Magnitude and Quality of Immune Responses

Author

Peter Dawson, Jaranit Kaewkungwal, Faruk Sinangil, Elizabeth Heger, Lindsay Wieczorek, James Tartaglia, Punnee Pitisuttithum, Rv Study Team, Alexandra Schuetz, Sanjay Phogat, Carlos A. DiazGranados, Suwat Chariyalertsak, Nelson L. Michael, Kirsten S. Smith, Merlin L. Robb, Jerome H. Kim, Victoria R. Polonis, Siriwat Akapirat, Benjaluck Phonrat, Surat Jongrakthaitae, Sandhya Vasan, Michael A. Eller, Yingjun Zhou, Dohoon Kim, Robert J. O'Connell, Nicos Karasavvas, Jittima Dhitavat, Jean-Louis Excler, Sorachai Nitayapha, and Poonam Pegu

Subjects

medicine.medical_specialty, Boosting (doping), business.industry, Public health, Declaration, Vaccine trial, Vaccine efficacy, law.invention, Regimen, Immune system, Randomized controlled trial, law, Family medicine, medicine, business

Abstract

Background: The RV144 phase 3 vaccine trial in Thailand demonstrated that ALVAC-HIV (vCP1521) and AIDSVAX® B/E administration over six months resulted in a 31% efficacy in preventing HIV acquisition. Subsequent boosting of RV144 vaccine recipients 6 to 8 years later improved the magnitude and quality of immune responses, expanding subdominant memory B cells. Methods: RV306 is a double-blind, placebo-controlled, randomized clinical trial of the primary RV144 vaccine series with additional AIDSVAX® B/E with or without ALVAC-HIV boosting at months 12, 15, or 18 in healthy volunteers. Findings: Late boosting was safe, and improved antigen-specific plasma IgG responses to HIV-1 envelope and the first and second variable loops (V1V2), an inverse correlate of HIV risk in RV144, without increasing HIV-specific plasma IgA, a direct correlate of risk. Late boosting improved Tier 1 neutralization and HIV-1 envelope-specific CD4+ T cell polyfunctionality, an independent correlate contributing to RV144 vaccine efficacy. Late boosting was also required to maintain antigen-specific CD4+ T cell proliferation. Interestingly, increasing the interval between priming and boosting improved several humoral and cellular immune responses. Interpretation: Taken together, these results suggest that additional boosting of the RV144 regimen with longer intervals between the primary vaccination series and late boost improved immune responses and may improve the efficacy of preventing HIV acquisition. Funding Statement: Cooperative Agreement # W81XWH-18-2-0040 in collaboration with the US Army and DAIDS/NIAID/NIH. Declaration of Interests: J. T., and C. D. are employees of Sanofi Pasteur. S.P. was an employee of Sanofi Pasteur during the conduct of this study and analysis. F. S. is an employee of Global Solutions for Infectious Diseases. All other authors report no potential conflicts. The opinions expressed herein are those of the authors and do not represent the official position of the US Army or the Department of Defense. Trade names are used for identification purposes only and do not imply endorsement. Ethics Approval Statement: The study was approved by ethical review boards at the Walter Reed Army Institute of Research, Thai Ministry of Public Health, Royal Thai Army Medical Department, Faculty of Tropical Medicine, Mahidol University, Chiang Mai University, and Chulalongkorn University Faculty of Medicine. This study was conducted in accordance with Good Participatory Practice principles.

Published

2019

32. Fluzone® High-Dose Influenza Vaccine

Author

David P. Greenberg, Ayman Chit, Corwin A. Robertson, Monica Mercer, Michael D. Decker, and Carlos A. DiazGranados

Subjects

0301 basic medicine, Canada, Influenza vaccine, Cost-Benefit Analysis, 030106 microbiology, Immunology, Hemagglutinin (influenza), Antibodies, Viral, 03 medical and health sciences, 0302 clinical medicine, Influenza, Human, Drug Discovery, Product Surveillance, Postmarketing, Humans, Medicine, Live attenuated influenza vaccine, 030212 general & internal medicine, Aged, Aged, 80 and over, Pharmacology, biology, business.industry, Immunogenicity, Immunosenescence, Middle Aged, Virology, United States, Hospitalization, Antibody response, Influenza Vaccines, biology.protein, Molecular Medicine, business

Abstract

Fluzone® High-Dose (IIV3-HD) is a trivalent, inactivated, split-virus influenza vaccine indicated for use in older adults (≥65 years of age). It contains 60 µg hemagglutinin of each influenza strain, which is four times the hemagglutinin content of standard-dose influenza vaccines, including Fluzone (IIV3-SD). IIV3-HD has been licensed for use in older adults in the US since December 2009 and in Canada since February 2016. Areas covered: In this review, we summarize postlicensure studies on the immunogenicity, safety, and effectiveness of IIV3-HD and estimates of its cost-effectiveness in older adults. We also discuss the potential application of IIV3-HD in adults 50-64 years of age and in individuals who may respond poorly to standard-dose influenza vaccines. Expert commentary: Multiple studies conducted since 2004 have consistently shown that, in older adults, IIV3-HD induces substantially greater antibody responses and better protection against influenza and influenza-associated hospitalization than IIV3-SD. Health economic analyses suggest that IIV3-HD can be a cost-effective alternative to standard-dose trivalent or quadrivalent inactivated influenza vaccines and can even be cost-saving compared to IIV3-SD in older adults. Further investigation of IIV3-HD vaccination as a way to improve immune responses and protection against influenza in immunocompromised individuals is warranted.

Published

2016

33. Correlates of Protection against Influenza in the Elderly: Results from an Influenza Vaccine Efficacy Trial

Author

Carlos A. DiazGranados, Andrew J. Dunning, H. Keipp Talbot, Branda Hu, Victoria Landolfi, and Timothy Voloshen

Subjects

0301 basic medicine, Microbiology (medical), Influenza vaccine, Clinical Biochemistry, Immunology, Neuraminidase, Antibodies, Viral, medicine.disease_cause, Virus, 03 medical and health sciences, Influenza A Virus, H1N1 Subtype, 0302 clinical medicine, Double-Blind Method, Influenza, Human, Influenza A virus, Humans, Immunology and Allergy, Medicine, 030212 general & internal medicine, Spotlight, Aged, Aged, 80 and over, Vaccines, Hemagglutination assay, biology, business.industry, Influenza A Virus, H3N2 Subtype, Antibody titer, Vaccine efficacy, Virology, Titer, 030104 developmental biology, Vaccines, Inactivated, Influenza Vaccines, biology.protein, Antibody, business

Abstract

Although a number of studies have investigated and quantified immune correlates of protection against influenza in adults and children, data on immune protection in the elderly are sparse. A recent vaccine efficacy trial comparing standard-dose with high-dose inactivated influenza vaccine in persons 65 years of age and older provided the opportunity to examine the relationship between values of three immunologic assays and protection against community-acquired A/H3N2 influenza illness. The high-dose vaccine induced significantly higher antibody titers than the standard-dose vaccine for all assays. For the hemagglutination inhibition assay, a titer of 40 was found to correspond with 50% protection when the assay virus was antigenically well matched to the circulating virus—the same titer as is generally recognized for 50% protection in younger adults. A dramatically higher titer was required for 50% protection when the assay virus was a poor match to the circulating virus. With the well-matched virus, some protection was seen at the lowest titers; with the poorly matched virus, high levels of protection were not achieved even at the highest titers. Strong associations were also seen between virus neutralization test titers and protection, but reliable estimates for 50% protection were not obtained. An association was seen between titers of an enzyme-linked lectin assay for antineuraminidase N2 antibodies and protection; in particular, the proportion of treatment effect explained by assay titer in models that included both this assay and one of the other assays was consistently higher than in models that included either assay alone. (This study has been registered at ClinicalTrials.gov under registration no. NCT01427309.)

Published

2016

34. Effect of Previous-Year Vaccination on the Efficacy, Immunogenicity, and Safety of High-Dose Inactivated Influenza Vaccine in Older Adults

Author

Corwin A. Robertson, H. Keipp Talbot, Carlos A. DiazGranados, Andrew J. Dunning, Victoria Landolfi, and David P. Greenberg

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Influenza vaccine, 030106 microbiology, Context (language use), human influenza vaccines, inactivated vaccines, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, law, age 80 and older, Internal medicine, Influenza prevention, Medicine, Live attenuated influenza vaccine, 030212 general & internal medicine, Articles and Commentaries, phase 3 clinical trial, business.industry, Immunogenicity, Vaccine efficacy, Vaccination, aged, Infectious Diseases, Immunology, business

Abstract

High-dose inactivated split-virus influenza vaccine showed higher immunogenicity and relative efficacy compared with standard-dose inactivated split-virus influenza vaccine, irrespective of type of vaccine used the preceding year. The safety profile was also unaffected by previous-year vaccine., Background. High-dose inactivated influenza vaccine (IIV-HD) is an alternative to the standard-dose inactivated influenza vaccine (IIV-SD) in the United States for influenza prevention in older adults. IIV-HD improved efficacy relative to IIV-SD in a randomized controlled trial. Recent observational studies suggest that previous influenza vaccination may influence the immunogenicity and effectiveness of current-season vaccination. Methods. The original study was a double-blind, randomized trial comparing IIV-HD to IIV-SD in adults aged ≥65 years over 2 influenza seasons. A subset of year 1 (Y1) participants reenrolled in year 2 (Y2), receiving vaccine by random assignment in both years. We evaluated the effect of Y1 vaccination on Y2 relative vaccine efficacy (VE), immunogenicity (hemagglutination inhibition [HAI] titers), and safety among reenrolled participants. Results. Of 14 500 Y1 participants, 7643 reenrolled in Y2. Relative to participants who received IIV-SD both seasons, VE was higher for IIV-HD vaccinees in Y2 (28.3% overall; 25.1% for Y1 IIV-HD, Y2 IIV-HD; and 31.6% for Y1 IIV-SD, Y2 IIV-HD). In multivariate logistic regression models, Y1 vaccine was not a significant modifier of Y2 VE (P = .43), whereas Y2 IIV-HD remained significantly associated with lower influenza risk (P = .043). Compared to administration of IIV-SD in both years, postvaccination HAI titers were significantly higher for patterns that included IIV-HD in Y2. No safety concerns were raised with IIV-HD revaccination. Conclusions. IIV-HD is likely to provide clinical benefit over IIV-SD irrespective of previous-season vaccination with IIV-HD or IIV-SD. IIV-HD consistently improved immune responses, and no safety concerns emerged in the context of IIV-HD revaccination.

Published

2016

35. Evaluation of dengue serological tests available in Puerto Rico for identification of prior dengue infection for prevaccination screening

Author

Yaniv Lustig, Lingyi Zheng, Matthew Bonaparte, Carlos A. DiazGranados, Shekema Hodge, James Huleatt, Stephen Savarino, and Yasemin Ataman-Önal

Subjects

0301 basic medicine, Microbiology (medical), 030106 microbiology, Dengue Vaccines, Enzyme-Linked Immunosorbent Assay, Cross Reactions, Antibodies, Viral, Sensitivity and Specificity, Serology, Dengue fever, Dengue, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, Humans, Medicine, Serologic Tests, 030212 general & internal medicine, Clinical Trials as Topic, Rapid diagnostic test, Zika Virus Infection, business.industry, Puerto Rico, Vaccination, General Medicine, medicine.disease, Virology, Infectious Diseases, Immunoglobulin M, Immunoglobulin G, business

Abstract

We assessed a dengue IgG rapid diagnostic test (RDT) and IgG enzyme-linked immunosorbent assay (ELISA) to determine their suitability for dengue prevaccination screening. Each exhibited ≥99% specificity. The RDT demonstrated no Zika cross-reactivity, while the ELISA displayed greater sensitivity. Both could safely guide vaccination in Puerto Rico pending availability of improved serotests.

Published

2020

36. Prevention of M. tuberculosis Infection with H4:IC31 Vaccine or BCG Revaccination

Author

Elisa, Nemes, Hennie, Geldenhuys, Virginie, Rozot, Kathryn T, Rutkowski, Frances, Ratangee, Nicole, Bilek, Simbarashe, Mabwe, Lebohang, Makhethe, Mzwandile, Erasmus, Asma, Toefy, Humphrey, Mulenga, Willem A, Hanekom, Steven G, Self, Linda-Gail, Bekker, Robert, Ryall, Sanjay, Gurunathan, Carlos A, DiazGranados, Peter, Andersen, Ingrid, Kromann, Thomas, Evans, Ruth D, Ellis, Bernard, Landry, David A, Hokey, Robert, Hopkins, Ann M, Ginsberg, Thomas J, Scriba, Mark, Hatherill, and Noncedo, Xoyana

Subjects

0301 basic medicine, Male, Tuberculosis, Adolescent, Immunization, Secondary, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Tuberculosis diagnosis, Medicine, Humans, 030212 general & internal medicine, Seroconversion, Child, Tuberculosis Vaccines, Proportional Hazards Models, Vaccines, biology, business.industry, General Medicine, biology.organism_classification, medicine.disease, Antibodies, Bacterial, Vaccination, 030104 developmental biology, Immunization, Immunology, BCG Vaccine, Female, Tuberculosis vaccines, business, BCG vaccine, Research Article

Abstract

Recent Mycobacterium tuberculosis infection confers a predisposition to the development of tuberculosis disease, the leading killer among global infectious diseases. H4:IC31, a candidate subunit vaccine, has shown protection against tuberculosis disease in preclinical models, and observational studies have indicated that primary bacille Calmette-Guérin (BCG) vaccination may offer partial protection against infection.In this phase 2 trial, we randomly assigned 990 adolescents in a high-risk setting who had undergone neonatal BCG vaccination to receive the H4:IC31 vaccine, BCG revaccination, or placebo. All the participants had negative results on testing for M. tuberculosis infection on the QuantiFERON-TB Gold In-tube assay (QFT) and for the human immunodeficiency virus. The primary outcomes were safety and acquisition of M. tuberculosis infection, as defined by initial conversion on QFT that was performed every 6 months during a 2-year period. Secondary outcomes were immunogenicity and sustained QFT conversion to a positive test without reversion to negative status at 3 months and 6 months after conversion. Estimates of vaccine efficacy are based on hazard ratios from Cox regression models and compare each vaccine with placebo.Both the BCG and H4:IC31 vaccines were immunogenic. QFT conversion occurred in 44 of 308 participants (14.3%) in the H4:IC31 group and in 41 of 312 participants (13.1%) in the BCG group, as compared with 49 of 310 participants (15.8%) in the placebo group; the rate of sustained conversion was 8.1% in the H4:IC31 group and 6.7% in the BCG group, as compared with 11.6% in the placebo group. Neither the H4:IC31 vaccine nor the BCG vaccine prevented initial QFT conversion, with efficacy point estimates of 9.4% (P=0.63) and 20.1% (P=0.29), respectively. However, the BCG vaccine reduced the rate of sustained QFT conversion, with an efficacy of 45.4% (P=0.03); the efficacy of the H4:IC31 vaccine was 30.5% (P=0.16). There were no clinically significant between-group differences in the rates of serious adverse events, although mild-to-moderate injection-site reactions were more common with BCG revaccination.In this trial, the rate of sustained QFT conversion, which may reflect sustained M. tuberculosis infection, was reduced by vaccination in a high-transmission setting. This finding may inform clinical development of new vaccine candidates. (Funded by Aeras and others; C-040-404 ClinicalTrials.gov number, NCT02075203 .).

Published

2018

37. Gastrointestinal Events in High-Dose vs Standard-Dose Influenza Vaccine Recipients

Author

Victoria Landolfi, David P. Greenberg, Andrew J. Dunning, Carlos A. DiazGranados, Corwin A. Robertson, and H. Keipp Talbot

Subjects

high-dose, medicine.medical_specialty, Influenza vaccine, business.industry, Brief Report, gastrointestinal side effects, vaccination, law.invention, Vaccination, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Oncology, Randomized controlled trial, law, 030225 pediatrics, Internal medicine, medicine, Epidemiological surveillance, 030212 general & internal medicine, Adverse effect, business, influenza

Abstract

Passive surveillance data had signaled the possibility of gastrointestinal adverse events occurring after the administration of high-dose inactivated influenza vaccine (IIV-HD). However, in a large, prospective randomized clinical trial, rates of serious gastrointestinal events were no greater among IIV-HD recipients than among those who received a standard-dose influenza vaccine.

Published

2018

38. Development of an anti-dengue NS1 IgG ELISA to evaluate exposure to dengue virus

Author

Ernesto T. A. Marques, Lingyi Zheng, Carlos A. DiazGranados, James Huleatt, Eduardo J. M. Nascimento, James K. George, Matthew Bonaparte, and Melissa Velasco

Subjects

0301 basic medicine, Adult, viruses, Yellow fever vaccine, Dengue Vaccines, Enzyme-Linked Immunosorbent Assay, Dengue virus, Viral Nonstructural Proteins, medicine.disease_cause, Antibodies, Viral, Sensitivity and Specificity, Virus, Dengue fever, Zika virus, 03 medical and health sciences, Virology, medicine, Humans, Dengue vaccine, Vaccines, Synthetic, biology, Yellow fever, Dengue Virus, biology.organism_classification, medicine.disease, Flavivirus, 030104 developmental biology, ROC Curve, Immunoglobulin G, medicine.drug

Abstract

Dengue virus infection elicits immune responses to multiple viral antigens including antibodies to dengue non-structural protein 1 (NS1) which are rapidly induced and detected within days of infection. The recombinant, live, attenuated, tetravalent dengue vaccine (CYD-TDV; Sanofi Pasteur) uses the yellow fever vaccine virus as a back-bone but expresses dengue virus pre-membrane and envelop proteins. Since CYD-TDV does not express dengue NS1, we evaluated the utility of dengue NS1-specific IgG antibodies as biomarkers of dengue exposure in CYD-TDV recipients and controls. We optimized and evaluated a quantitative anti-dengue NS1 IgG enzyme-linked immunosorbent assay (ELISA). Parameters assessed included: accuracy, dilutability/linearity, precision, limit of quantitation and specificity. The assay specificity was further evaluated using Japanese Encephalitis virus, West Nile virus, Yellow Fever virus or Zika virus positive sera samples collected following confirmed infection or vaccination. Receiver-operating-characteristics (ROC) curves as well as sensitivity and specificity for discriminating previous dengue exposure were assessed using 1250 reference samples. Overall, the anti-dengue NS1 IgG ELISA was able to discriminate previous dengue exposure from non-exposure before vaccination with CYD-TDV (ROC area under the curve > 0.9). Assessment of paired samples from 2511 vaccinated participants showed high overall agreement (93%) between pre-vaccination and post-vaccination dengue serostatus classification based on the anti-dengue NS1 IgG ELISA. However, misclassification of dengue serostatus was observed after vaccination likely due to a combination of asymptomatic dengue infections, assay variability and a modest effect of CYD-TDV on the anti-dengue NS1 IgG ELISA readout.

Published

2018

39. Prevention of serious events in adults 65 years of age or older: A comparison between high-dose and standard-dose inactivated influenza vaccines

Author

David P. Greenberg, Corwin A. Robertson, H. Keipp Talbot, Victoria Landolfi, Carlos A. DiazGranados, and Andrew J. Dunning

Subjects

Male, medicine.medical_specialty, Drug-Related Side Effects and Adverse Reactions, Influenza vaccine, Influenza vaccines, human, Double-Blind Method, Internal medicine, Multicenter trial, Immunology and Microbiology(all), Influenza, Human, medicine, Humans, Adverse effect, Aged, Aged, 80 and over, General Veterinary, General Immunology and Microbiology, business.industry, Public Health, Environmental and Occupational Health, medicine.disease, Survival Analysis, veterinary(all), Confidence interval, Hospitalization, Pneumonia, Infectious Diseases, Vaccines, Inactivated, Influenza Vaccines, Immunology, Molecular Medicine, Female, Clinical trial, phase III, business

Abstract

Background A recent study showed that a high-dose inactivated influenza vaccine (IIV-HD) was 24.2% more efficacious than a standard-dose inactivated influenza vaccine (IIV-SD) in preventing laboratory-confirmed symptomatic influenza in adults ≥65 years. Here we evaluate the effectiveness of IIV-HD compared to IIV-SD in preventing serious illnesses considered potential sequelae or complications of influenza infection. Methods The original study was a double-blind, randomized, active-controlled, multicenter trial. Participants were adults ≥65 years randomized to receive IIV-HD or IIV-SD, and followed for 6–8 months post-vaccination for the occurrence of influenza and serious adverse events (SAEs). SAEs were events: leading to death or hospitalization (or its prolongation); considered life-threatening or medically important; or resulting in disability. For the present analysis, reported SAEs were classified as possibly related to influenza by three blinded physicians and rates per 1000 participant-seasons were calculated. Relative vaccine effectiveness (rVE) was estimated as (1 − Rate Ratio) × 100. Results 31,989 participants were enrolled, with 15,991 and 15,998 randomized to receive IIV-HD and IIV-SD, respectively. IIV-HD was significantly more effective than IIV-SD in preventing SAEs possibly related to influenza overall (rVE, 17.7%; 95% confidence interval [CI], 6.6–27.4%) and serious pneumonia (rVE, 39.8%; 95% CI, 19.3–55.1%). Borderline significance was observed for the efficacy of IIV-HD relative to IIV-SD for the prevention of all-cause hospitalizations (rVE, 6.9%; 95% CI, 0.5–12.8%). Conclusions Compared to IIV-SD, IIV-HD reduced the risk of SAEs possibly related to influenza. The observed relative effectiveness against serious pneumonia is particularly noteworthy considering the burden of influenza and pneumonia in older adults.

Published

2015

40. Efficacy and immunogenicity of high-dose influenza vaccine in older adults by age, comorbidities, and frailty

Author

H. Keipp Talbot, Victoria Landolfi, Corwin A. Robertson, Carlos A. DiazGranados, Andrew J. Dunning, and David P. Greenberg

Subjects

Male, medicine.medical_specialty, Influenza vaccine, Comorbidity, Antibodies, Viral, Influenza vaccines, human, law.invention, Double-Blind Method, Randomized controlled trial, law, Internal medicine, Multicenter trial, Immunology and Microbiology(all), Influenza, Human, medicine, Humans, Aged, Aged, 80 and over, Hemagglutination assay, General Veterinary, General Immunology and Microbiology, business.industry, Public Health, Environmental and Occupational Health, Hemagglutination Inhibition Tests, medicine.disease, Vaccine efficacy, veterinary(all), Confidence interval, Titer, Treatment Outcome, Infectious Diseases, Vaccines, Inactivated, Influenza Vaccines, Immunology, Molecular Medicine, Female, Clinical trial, phase III, business, Biomarkers, Follow-Up Studies

Abstract

Background A randomized trial demonstrated that a high-dose inactivated influenza vaccine (IIV-HD) was 24.2% more efficacious than a standard-dose vaccine (IIV-SD) against laboratory-confirmed influenza illness in adults ≥65 years. To evaluate the consistency of IIV-HD benefits, supplemental analyses explored efficacy and immunogenicity by baseline characteristics of special interest. Methods Double-blind, randomized, active-controlled, multicenter trial. Adults ≥65 years were randomized 1:1 to receive IIV-HD or IIV-SD and followed for 6–8 months postvaccination for the occurrence of influenza. One third of participants were randomly selected to provide sera for measurement of hemagglutination inhibition antibody (HAI) titers. Efficacy (IIV-HD vs. IIV-SD) against laboratory-confirmed, protocol-defined influenza-like illness (PD-ILI) and HAI geometric mean titer (GMT) ratios (IIV-HD/IIV-SD) were evaluated by age, and number of high-risk comorbid and frailty conditions. Results Efficacy (95% confidence intervals) of IIV-HD relative to IIV-SD against laboratory-confirmed PD-ILI was 19.7% (0.4%; 35.4%) for participants 65–74 years, 32.4% (8.1%; 50.6%) for those ≥75 years, 22.1% (3.9%; 37.0%) for participants with ≥1 high-risk comorbidity, 23.6% (−3.2%; 43.6%) for those with ≥2 high-risk comorbidities, 27.5% (0.4%; 47.4%) for persons with 1 frailty condition, 23.9% (−9.0%; 47.2%) for those with 2 frailty conditions, and 16.0% (−16.3%; 39.4%) for those with ≥3 frailty conditions. There was no evidence of vaccine efficacy heterogeneity within age, comorbidity, and frailty strata ( P -values 0.351, 0.875, and 0.838, respectively). HAI GMT ratios were significantly higher among IIV-HD recipients for all strains and across all subgroups. Conclusions Estimates of relative efficacy consistently favored IIV-HD over IIV-SD. There was no significant evidence that baseline age, comorbidity, or frailty modified the efficacy of IIV-HD relative to IIV-SD. IIV-HD significantly improved HAI responses for all strains and in all subgroups. IIV-HD is likely to provide benefits beyond IIV-SD for adults ≥65 years, irrespective of age and presence of comorbid or frailty conditions.

Published

2015

41. Immunogenicity and safety of Fluzone® intradermal and high-dose influenza vaccines in older adults ≥65 years of age: A randomized, controlled, phase II trial

Author

Peter H. Tsang, Cynthia Strout, Malcolm Sperling, Victoria Landolfi, Carlos A. DiazGranados, Ayca Ozol-Godfrey, Geoffrey J. Gorse, and David P. Greenberg

Subjects

Adult, Male, Trivalent influenza vaccine, Adolescent, Injections, Intradermal, Dose, Phases of clinical research, Hemagglutinin Glycoproteins, Influenza Virus, Antibodies, Viral, Injections, Intramuscular, Antibodies, Young Adult, Influenza A Virus, H1N1 Subtype, Intradermal, Immunology and Microbiology(all), Influenza, Human, Humans, Medicine, Seroconversion, Adverse effect, Aged, High-dose vaccine, General Veterinary, General Immunology and Microbiology, biology, business.industry, Influenza A Virus, H3N2 Subtype, Immunogenicity, Public Health, Environmental and Occupational Health, Middle Aged, veterinary(all), Influenza B virus, Titer, Infectious Diseases, Influenza Vaccines, Older adults, Immunology, biology.protein, Molecular Medicine, Female, Antibody, Safety, business

Abstract

We conducted a randomized, controlled, multicenter, phase II study to evaluate the immunogenicity and safety of an investigational intradermal (ID) trivalent influenza vaccine (TIV) and a high-dose (HD) intramuscular (IM) TIV in older adults (≥65 years of age). Older adult subjects were immunized with ID vaccine containing either 15μg hemagglutinin (HA)/strain (n=636) or 21μg HA/strain (n=634), with HD IM vaccine containing 60μg HA/strain (n=320), or with standard-dose (SD) IM vaccine (Fluzone®; 15μg HA/strain; n=319). For comparison, younger adults (18–49 years of age) were immunized with SD IM vaccine. In older adults, post-vaccination geometric mean titers induced by the ID vaccines were superior to those induced by the SD IM vaccine for the A/H1N1 and A/H3N2 strains and non-inferior for the B strain. Seroconversion rates induced by the ID vaccines were superior to those induced by the SD IM vaccine in older adults for the A/H1N1 and B strains and non-inferior for the A/H3N2 strain. Results did not differ significantly for the two ID vaccine dosages. Post-vaccination geometric mean titers, seroconversion rates, and most seroprotection rates were significantly higher in HD vaccine recipients than in older adult recipients of the SD IM or ID vaccines and, for most measures, were comparable to those of younger adult SD IM vaccine recipients. Injection-site reactions, but not systemic reactions or unsolicited adverse events, were more common with the ID vaccines than with the IM vaccines. No treatment-related serious adverse events were reported. This study demonstrated that: (1) the ID and HD vaccines were well-tolerated and more immunogenic than the SD IM vaccine in older adults; (2) the HD vaccine was more immunogenic than the ID vaccines in older adults; and (3) the HD vaccine in older adults and the SD IM vaccine in younger adults elicited comparable antibody responses (ClinicalTrials.gov identifier no.: NCT00551031).

Published

2014

42. High vancomycin minimum inhibitory concentration and clinical outcomes in adults with methicillin-resistant Staphylococcus aureus infections: a meta-analysis

Author

Carlos A. DiazGranados and Jesse T. Jacob

Subjects

Adult, Microbial sensitivity testing, Microbiology (medical), medicine.medical_specialty, Bacteremia, Microbial Sensitivity Tests, Staphylococcal infections, medicine.disease_cause, Article, 03 medical and health sciences, Minimum inhibitory concentration, 0302 clinical medicine, Vancomycin, Internal medicine, medicine, Humans, 030212 general & internal medicine, Mortality, Etest, 0303 health sciences, 030306 microbiology, business.industry, Broth microdilution, Vancomycin Resistance, General Medicine, Staphylococcal Infections, medicine.disease, Survival Analysis, Methicillin-resistant Staphylococcus aureus, Anti-Bacterial Agents, 3. Good health, Surgery, Treatment Outcome, Infectious Diseases, Relative risk, business, medicine.drug

Abstract

Summary Background Patients with methicillin-resistant Staphylococcus aureus (MRSA) infections caused by isolates with a high but ‘susceptible' minimum inhibitory concentration (MIC) to vancomycin may suffer poor outcomes. The aim of this study was to determine the association of high compared to low vancomycin MICs and clinical outcomes (treatment failure and mortality) in patients with MRSA infections. Methods PubMed, the Cochrane Library, and electronic abstracts from meetings were queried from January 2000 to July 2010. Two reviewers independently screened titles and abstracts of studies evaluating outcomes of patients with MRSA infections, using broth microdilution (BMD) or the Etest to determine MIC, for full-text review. Patients participating in included studies were classified into two mutually exclusive groups: high MIC or low MIC. High MIC was defined as MIC ≥1mg/l by BMD or ≥1.5mg/l by Etest. Study-defined failure and mortality were assessed in each group. Results Fourteen publications and six electronic abstracts met the inclusion criteria, with 2439 patients (1492 high MIC and 947 low MIC). There was no evidence of publication bias or heterogeneity. An increased risk of failure was observed in the high MIC group compared to the low MIC group (summary risk ratio (RR) 1.40, 95% confidence interval (CI) 1.15–1.71). The overall mortality risk was greater in the high MIC group than in the low MIC group (summary RR 1.42, 95% CI 1.08–1.87). Sensitivity analyses showed similar findings for failure (summary RR 1.37, 95% CI 1.09–1.73) and mortality (summary RR 1.46, 95% CI 1.06–2.01) for patients with bacteremia. The study quality was poor-to-moderate, and study-defined endpoints were variable. Conclusions A susceptible but high MIC to vancomycin is associated with increased mortality and treatment failure among patients with MRSA infections.

Published

2013

43. Seasonal influenza vaccine efficacy and its determinants in children and non-elderly adults: A systematic review with meta-analyses of controlled trials

Author

Carlos A. DiazGranados, Stanley A. Plotkin, and Martine Denis

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Influenza vaccine, Context (language use), Young Adult, Internal medicine, Influenza, Human, Influenza prevention, medicine, Humans, Child, General Veterinary, General Immunology and Microbiology, business.industry, Incidence (epidemiology), Public Health, Environmental and Occupational Health, Middle Aged, Vaccine efficacy, Vaccination, Infectious Diseases, Influenza Vaccines, Meta-analysis, Relative risk, Immunology, Molecular Medicine, Female, Controlled Clinical Trials as Topic, business

Abstract

Context The true level of influenza vaccine efficacy is controversial and many factors may influence its estimation. Objectives To estimate the efficacy of vaccination of children and non-elderly adults for the prevention of influenza and to explore the impact of type of vaccine, age, degree of strain matching, influenza type and case ascertainment methods on vaccine efficacy estimates. Data sources Medline and EmBase databases until October 2011. References of relevant articles were also reviewed. Study selection Controlled trials evaluating seasonal influenza vaccines and presenting incidence of laboratory-confirmed influenza illness were eligible. Studies exploring efficacy after experimental challenge, presenting duplicate data, employing group randomization, or focusing on special populations were excluded. Data extraction The vaccine effect on influenza prevention was evaluated by calculating Mantel–Haenszel risk ratios (RR) and using random-effects models. Vaccine efficacies were calculated for each comparison as (1 − RR) × 100. Results Thirty studies were included in one or more of a total of 101 analyses, comprising 88.468 study participants. There was evidence of heterogeneity in 49% of the analyses. Summary vaccine efficacy was 65% against any strain, 78% against matched strains and 55% against not-matched strains. Both live-attenuated and inactivated vaccines showed similar levels of protection against not-matched strains (60% and 55%, respectively). Live-attenuated vaccines performed better than inactivated vaccines in children (80% versus 48%), whereas inactivated vaccines performed better than live-attenuated vaccines in adults (59% versus 39%). There was a large difference (20%) in efficacy against influenza A (69%) and influenza B (49%) types for not-matched strains. Summary estimates of vaccine efficacy were highest when ascertainment was based on culture confirmation. Conclusion Influenza vaccines are efficacious, but efficacy estimates depend on many variables including type of vaccine and age of vaccinees, degree of matching of the circulating strains to the vaccine, influenza type, and methods of case ascertainment.

Published

2012

44. High-Dose Inactivated Influenza Vaccine is Associated with Cost Savings and Better Outcomes Compared to Standard-Dose Inactivated Influenza Vaccine in Canadian Seniors

Author

Carlos A. DiazGranados, Eddy Yau, Michael Drummond, Ayman Chit, Michael Maschio, and Debbie L. Becker

Subjects

Male, medicine.medical_specialty, Canada, Influenza vaccine, Cost effectiveness, Total cost, Cost-Benefit Analysis, 030231 tropical medicine, Immunology, Seasonal influenza, 03 medical and health sciences, 0302 clinical medicine, Cost Savings, Health care, Influenza, Human, medicine, Immunology and Allergy, Humans, 030212 general & internal medicine, Intensive care medicine, cost-utility, cost-effectiveness, health care economics and organizations, Aged, Pharmacology, Aged, 80 and over, business.industry, high-dose inactivated influenza vaccine, Fluzone, Research Papers, Cost savings, Clinical trial, Treatment Outcome, Vaccines, Inactivated, Influenza Vaccines, Emergency medicine, Quality of Life, Female, business, influenza, Resource utilization

Abstract

Seasonal influenza infects approximately 10–20% of Canadians each year, causing an estimated 12,200 hospitalizations and 3,500 deaths annually, mostly occurring in adults ≥65 years old (seniors). A 32,000-participant, randomized controlled clinical trial (FIM12; Clinicaltrials.gov NCT01427309) showed that high-dose inactivated influenza vaccine (IIV-HD) is superior to standard-dose vaccine (SD) in preventing laboratory-confirmed influenza illness in seniors. In this study, we performed a cost-utility analysis (CUA) of IIV-HD versus SD in FIM12 participants from a Canadian perspective. Healthcare resource utilization data collected in FIM12 included: medications, non-routine/urgent care and emergency room visits, and hospitalizations. Unit costs were applied using standard Canadian cost sources to estimate the mean direct medical and societal costs associated with each vaccine (2014 CAD). Clinical illness data from the trial were mapped to quality-of-life data from the literature to estimate differences in effectiveness between vaccines. Time horizon was one influenza season, however, quality-adjusted life-years (QALYs) lost due to death during the study were captured over a lifetime. A probabilistic sensitivity analysis (PSA) was also performed. Average per-participant medical costs were $47 lower and societal costs $60 lower in the IIV-HD arm. Hospitalizations contributed 91% of the total cost and were less frequent in the IIV-HD arm. IIV-HD provided a gain in QALYs and, due to cost savings, dominated SD in the CUA. The PSA indicated that IIV-HD is 89% likely to be cost saving. In Canada, IIV-HD is expected to be a less costly and more effective alternative to SD, driven by a reduction in hospitalizations.

Published

2016

45. Selection of HIV Vaccine Candidates for Concurrent Testing in an Efficacy Trial

Author

Ying Huang, Susan Buchbinder, Peter B. Gilbert, Patricia Bourguignon, Barbara Metch, Carlos A. DiazGranados, Allan C. deCamp, Brittany Sanchez, Georgia D. Tomaras, Marguerite Koutsoukos, Niranjan Kanesa-thasan, Lawrence Corey, Alix Collard, J. McElrath, Shannon Grant, James G. Kublin, Yunda Huang, Sanjay Phogat, Glenda Gray, and Holly Janes

Subjects

0301 basic medicine, medicine.medical_specialty, HIV Infections, Concurrent testing, Bioinformatics, Article, 03 medical and health sciences, 0302 clinical medicine, Immunogenicity, Vaccine, Virology, medicine, Humans, 030212 general & internal medicine, HIV vaccine, Intensive care medicine, Vaccine Potency, Selection (genetic algorithm), Immunization Schedule, AIDS Vaccines, Clinical Trials as Topic, business.industry, Extramural, Data interpretation, Vaccine efficacy, 030104 developmental biology, Data Interpretation, Statistical, HIV-1, business, Algorithms

Abstract

Phase IIb or III HIV-1 vaccine efficacy trials are generally large and operationally challenging. To mitigate this challenge, the HIV Vaccine Trials Network is designing a Phase IIb efficacy trial accommodating the evaluation of multiple vaccine regimens concurrently. As this efficacy trial would evaluate a limited number of vaccine regimens, there is a need to develop a framework for optimizing the strategic selection of regimens from the large number of vaccine candidates tested in Phase I/IIa trials. In this paper we describe the approaches for the selection process, including the choice of immune response endpoints and the statistical criteria and algorithms. We illustrate the selection approaches using data from HIV-1 vaccine trials.

Published

2016

46. Prospective audit for antimicrobial stewardship in intensive care: Impact on resistance and clinical outcomes

Author

Carlos A. DiazGranados

Subjects

Adult, Male, medicine.medical_specialty, Georgia, Critical Care, Epidemiology, Critical Illness, Pharmacist, Drug resistance, Audit, Drug Prescriptions, Intensive care, Medication therapy management, medicine, Humans, Antimicrobial stewardship, Prospective Studies, Medical prescription, Aged, business.industry, Health Policy, Public Health, Environmental and Occupational Health, Health services research, Bacterial Infections, Middle Aged, Drug Utilization, Hospitals, Anti-Bacterial Agents, Intensive Care Units, Treatment Outcome, Infectious Diseases, Emergency medicine, Female, Health Services Research, business

Abstract

Background The impact of antimicrobial audit and feedback on outcomes of critically ill adults is unclear. Methods A prospective study was performed in the intensive care units (ICU) of a public hospital in Atlanta, GA. Critically ill adults receiving empiric imipenem or piperacillin-tazobactam were eligible. Outcomes for 3 periods were compared: baseline (B, February to May 2006), model 1 (M1, October 2006 to July 2008), and model 2 (M2, September 2008 to February 2009). No audit was performed during B. During M1, an infectious diseases physician evaluated patients, and a critical care pharmacist communicated recommendations to the treating team. During M2, an infectious diseases physician directly participated in interdisciplinary rounds with the medical ICU team. Results One hundred ninety-four patients were included during B, 415 during M1, and 83 during M2. M1 and M2 were associated with appropriate antimicrobial selection (B, 70%; M1, 78%; M2, 82%; P = .042) and with lower rates of resistance (B, 31%; M1, 25%; M2, 17%; P = .033). Logistic regression analysis confirmed that audit and feedback were independently associated with appropriate antimicrobial selection and prevention of resistance. The association remained strongest for M2. Conclusion Audit and feedback had an influence on antimicrobial prescription patterns in the ICU with a favorable impact on the emergence of resistance.

Published

2012

47. Rate and predictors of optimal virologic response to antiretroviral therapy in Colombia

Author

Monica Mantilla, Diana Roncancio, Alfonso Silva, Carlos A. DiazGranados, Pierina Diruggiero, and Adriana Bermudez

Subjects

Adult, Male, Microbiology (medical), medicine.medical_specialty, Multivariate analysis, Adolescent, HIV Infections, Colombia, Logistic regression, Developing countries, Cohort Studies, Internal medicine, Humans, Medicine, Viral load, Child, Retrospective Studies, Response rate (survey), business.industry, HIV, Retrospective cohort study, General Medicine, Middle Aged, Confidence interval, Antiretroviral therapy, Surgery, Regimen, Logistic Models, Latin America, Infectious Diseases, Anti-Retroviral Agents, Child, Preschool, Multivariate Analysis, Female, business, Cohort study

Abstract

Summary Objective To estimate the rate of optimal response to antiretroviral therapy and its predictors in Colombia. Methods A retrospective cohort study was performed. The medical records of all patients at three major HIV clinics in different areas of Colombia, South America, were reviewed. Eligible patients met the following criteria: (1) viral load test available while on therapy; and (2) patients must have been on a stable first antiviral regimen for at least 1 year (48 weeks). Optimal virologic response was defined as a viral load Results Two hundred and twenty patients were eligible for the study. The optimal virologic response rate was 40% (95% confidence interval 34–46%). Younger age ( p =0.02) and western region of the country ( p =0.026) were the only significant predictors of non-optimal response in bivariate analysis. Multivariate logistic regression analysis confirmed younger age ( p =0.0054) and geographic area ( p =0.0468) as independent predictors of non-optimal response. Conclusions The optimal response rate in some areas of Colombia seems lower than that reported for other areas of the developing world. Poorer virologic responses were observed in younger patients and in those from the western region of the country.

Published

2007

48. Cost-effectiveness of high-dose versus standard-dose inactivated influenza vaccine in adults aged 65 years and older: an economic evaluation of data from a randomised controlled trial

Author

Eddy Yau, Michael Drummond, Carlos A. DiazGranados, Debbie L. Becker, Ayman Chit, and Michael Maschio

Subjects

Male, Pediatrics, medicine.medical_specialty, Cost effectiveness, Influenza vaccine, Cost-Benefit Analysis, law.invention, Randomized controlled trial, law, Influenza, Human, medicine, Humans, Resource consumption, Immunization Schedule, Aged, Aged, 80 and over, Models, Statistical, business.industry, Cost savings, Hospitalization, Infectious Diseases, Influenza A virus, Influenza Vaccines, Economic evaluation, Vaccines, Subunit, Population study, Female, Quality-Adjusted Life Years, business, Medical costs

Abstract

Summary Background Adults aged 65 years and older account for most seasonal influenza-related hospital admissions and deaths. Findings from the randomised controlled FIM12 study showed that high-dose inactivated influenza vaccine is more effective than standard-dose vaccine for prevention of laboratory-confirmed influenza in this age group. We aimed to assess the economic impact of high-dose versus standard-dose influenza vaccine in participants in the FIM12 study population. Methods The FIM12 study was a head-to-head randomised controlled trial in which 31 989 participants aged 65 years and older were randomly assigned (1:1) to receive either high-dose or standard-dose trivalent inactivated influenza vaccine over two influenza seasons (2011–12 and 2012–13). Data for health-care resource consumption obtained in the FIM12 study were summarised across vaccine groups. Unit costs obtained from standard US cost sources were applied to each resource item, including to the vaccines (high dose US$31·82, standard dose $12·04). Clinical illness data were mapped to existing quality-of-life data. The time horizon was one influenza season; however, quality-adjusted life-years (QALYs) lost due to death during the study were calculated over a lifetime. We calculated incremental cost-effectiveness ratios (ICERs) for high-dose versus standard-dose vaccine and used QALYs as an outcome in the cost-utility analysis. We undertook a probabilistic sensitivity analysis using bootstrapping to explore the effect of statistical uncertainty on the study results. Findings Mean per-participant medical costs were lower in the high-dose vaccine group ($1376·72 [SD 6857·59]) than in the standard-dose group ($1492·64 [7447·14]; difference –$115·92 [95% CI −264·18 to 35·48]). Mean societal costs were likewise lower in the high-dose versus the standard-dose group ($1506·48 [SD 7305·19] vs $1634·50 [7952·99]; difference −$128·02 [95% CI −286·89 to 33·30]). Hospital admissions contributed 95% of the total health-care-payer cost and 87% of the total societal costs. The mean per-participant number of hospital admissions was 0·0937 (SD 0·3644) in the high-dose group and 0·1017 (0·3708) in the standard-dose group (difference −0·0080, 95% CI −0·0160 to −0·0003). The high-dose vaccine provided a gain in QALYs (mean 8·1502 QALYs gained per participant [SD 0·5693]) compared with the standard-dose vaccine (8·1499 QALYs [0·5697]) and, due to cost savings, dominated standard-dose vaccine in the cost-utility analysis. The probabilistic sensitivity analysis showed that the high-dose vaccine is 93% likely to be cost saving. Interpretation High-dose trivalent inactivated influenza vaccine is a less costly and more effective alternative to the standard-dose vaccine, driven by a reduction in the number of hospital admissions. These findings are relevant to US health-care beneficiaries, providers, payers, and recommending bodies, especially those seeking to improve outcomes while containing costs. Funding Sanofi Pasteur.

Published

2015

49. Safety and immunogenicity of high-dose trivalent inactivated influenza vaccine in adults 50-64 years of age

Author

William Saway, Emilia Jordanov, Victoria Landolfi, Eddy Yau, Carlos A. DiazGranados, James Gouaux, Mira Baron, Martine Denis, and Jeffrey P. Baker

Subjects

Trivalent influenza vaccine, Male, medicine.medical_specialty, Drug-Related Side Effects and Adverse Reactions, Influenza vaccine, Antibodies, Viral, Internal medicine, Immunology and Microbiology(all), Influenza, Human, Medicine, Humans, Single-Blind Method, Seroconversion, Adverse effect, Hemagglutination assay, Reactogenicity, General Veterinary, General Immunology and Microbiology, business.industry, Immunogenicity, Public Health, Environmental and Occupational Health, Inactivated, Hemagglutination Inhibition Tests, Middle Aged, veterinary(all), Phase II, Vaccination, Clinical trial, Infectious Diseases, Treatment Outcome, Vaccines, Inactivated, Influenza Vaccines, Immunology, Molecular Medicine, Female, Safety, business

Abstract

Background Individuals 50–64 years of age have reduced immune responses to influenza vaccines. The current study examined whether a high-dose inactivated trivalent influenza vaccine (IIV3-HD) might improve immune responses over a standard-dose inactivated influenza vaccine (IIV3-SD) in this age group. Methods This was a multicenter, observer-blinded, randomized, active-controlled phase II trial. Adults 50–64 years of age were randomized 1:1 to receive IIV3-HD or IIV3-SD. Hemagglutination inhibition titers were measured before and 28 days after vaccination. Reactogenicity was recorded for 7 days after vaccination and adverse events for 28 days. Results 148 participants received IIV3-HD and 152 received IIV3-SD. For all vaccine strains, day 28 geometric mean hemagglutination inhibition titers were significantly higher in the IIV3-HD group than in the IIV3-SD group (geometric mean titer ratio [95% confidence interval (CI)] = 1.43 [1.04–1.97] for A/H1N1, 1.65 [1.21–2.25] for A/H3N2, and 1.60 [1.23–2.08] for B). Seroconversion rates were significantly higher in the IIV3-HD group than in the IIV3-SD group for strains A/H3N2 and B but not A/H1N1 (difference [95% CI] = 13.5% [4.76–22.0] for A/H3N2, 23.1% [11.7–33.6] for B, and −0.2% [−9.66 to 9.18] for A/H1N1). The post-vaccination seroprotection rate was significantly higher in the IIV3-HD group than in the IIV3-SD group for strain B but not for strains A/H1N1 or A/H3N2 (difference = 9.1% [2.95–15.7] for B, 2.0% [−0.907 to 5.68] for A/H1N1, and 0.6% [−3.14 to 4.43] for A/H3N2). Reactogenicity was higher in the IIV3-HD group than in the IIV3-SD group, but reactions were mostly of low intensity, transient, and self-limited. Rates of unsolicited adverse events were similar between groups. No serious AEs, AEs leading to early withdrawal, or deaths were reported. Conclusions The study suggests that in adults 50–64 years of age, IIV3-HD may improve immunogenicity compared to IIV3-SD while maintaining an acceptable safety profile.

Published

2015

50. Transmission of West Nile Virus from an Organ Donor to Four Transplant Recipients

Author

Susan E. Lance-Parker, Mary E. Chamberland, Andrea G Winquist, Walter C. Hellinger, Carlos A. DiazGranados, Jesse L. Goodman, Si M. Pham, Martha Iwamoto, Daniel B. Jernigan, Carl A Perlino, Carina Blackmore, Mary Jo Trepka, Steven T. Wiersma, Anthony A. Marfin, Krista L Hillyer, Robert S. Lanciotti, Lyle R. Petersen, Sherif R. Zaki, and Antonio Guasch

Subjects

Adult, Male, medicine.medical_specialty, viruses, Blood Donors, Antibodies, Viral, Organ transplantation, Central nervous system disease, Fatal Outcome, Blood-Borne Pathogens, Humans, Medicine, Viremia, Aged, biology, business.industry, Transmission (medicine), Transfusion Reaction, virus diseases, Organ Transplantation, General Medicine, Middle Aged, medicine.disease, Kidney Transplantation, Virology, Tissue Donors, Liver Transplantation, Transplantation, Immunoglobulin M, biology.protein, Heart Transplantation, Female, Viral disease, Antibody, Complication, business, West Nile virus, West Nile Fever, Encephalitis

Abstract

In August 2002, fever and mental-status changes developed in recipients of organs from a common donor. Transmission of West Nile virus through organ transplantation was suspected.We reviewed medical records, conducted interviews, and collected blood and tissue samples for testing with a variety of assays. Persons who donated blood to the organ donor and associated blood components were identified and tested for West Nile virus.We identified West Nile virus infection in the organ donor and in all four organ recipients. Encephalitis developed in three of the organ recipients, and febrile illness developed in one. Three recipients became seropositive for West Nile virus IgM antibody; the fourth recipient had brain tissue that was positive for West Nile virus by isolation and nucleic acid and antigen assays. Serum specimens obtained from the organ donor before and immediately after blood transfusions showed no evidence of West Nile virus; however, serum and plasma samples obtained at the time of organ recovery were positive on viral nucleic acid testing and viral culture. The organ donor had received blood transfusions from 63 donors. A review of blood donors and follow-up testing identified one donor who had viremia at the time of donation and who became seropositive for West Nile virus IgM antibodies during the next two months.Our investigation of this cluster documents the transmission of West Nile virus by organ transplantation. Organ recipients receiving immunosuppressive drugs may be at high risk for severe disease after West Nile virus infection. Blood transfusion was the probable source of the West Nile virus viremia in the organ donor.

Published

2003