Your search keyword '"Hural, John"' showing total 4 results

1. Pharmacokinetic serum concentrations of VRC01 correlate with prevention of HIV-1 acquisition.

Author

Seaton, Kelly, Seaton, Kelly, Huang, Yunda, Karuna, Shelly, Heptinstall, Jack, Brackett, Caroline, Chiong, Kelvin, Zhang, Lily, Yates, Nicole, Sampson, Mark, Rudnicki, Erika, Juraska, Michal, deCamp, Allan, Edlefsen, Paul, Mullins, James, Williamson, Carolyn, Rossenkhan, Raabya, Giorgi, Elena, Kenny, Avi, Angier, Heather, Randhawa, April, Weiner, Joshua, Rojas, Michelle, Sarzotti-Kelsoe, Marcella, Zhang, Lu, Sawant, Sheetal, Ackerman, Margaret, McDermott, Adrian, Mascola, John, Hural, John, McElrath, M, Andrew, Philip, Hidalgo, Jose, Laher, Fatima, Orrell, Catherine, Frank, Ian, Gonzales, Pedro, Edupuganti, Srilatha, Mgodi, Nyaradzo, Corey, Lawrence, Morris, Lynn, Montefiori, David, Cohen, Myron, Gilbert, Peter, Tomaras, Georgia, Clark, Jesse, Seaton, Kelly, Seaton, Kelly, Huang, Yunda, Karuna, Shelly, Heptinstall, Jack, Brackett, Caroline, Chiong, Kelvin, Zhang, Lily, Yates, Nicole, Sampson, Mark, Rudnicki, Erika, Juraska, Michal, deCamp, Allan, Edlefsen, Paul, Mullins, James, Williamson, Carolyn, Rossenkhan, Raabya, Giorgi, Elena, Kenny, Avi, Angier, Heather, Randhawa, April, Weiner, Joshua, Rojas, Michelle, Sarzotti-Kelsoe, Marcella, Zhang, Lu, Sawant, Sheetal, Ackerman, Margaret, McDermott, Adrian, Mascola, John, Hural, John, McElrath, M, Andrew, Philip, Hidalgo, Jose, Laher, Fatima, Orrell, Catherine, Frank, Ian, Gonzales, Pedro, Edupuganti, Srilatha, Mgodi, Nyaradzo, Corey, Lawrence, Morris, Lynn, Montefiori, David, Cohen, Myron, Gilbert, Peter, Tomaras, Georgia, and Clark, Jesse

Abstract

BACKGROUND: The phase 2b proof-of-concept Antibody Mediated Prevention (AMP) trials showed that VRC01, an anti-HIV-1 broadly neutralising antibody (bnAb), prevented acquisition of HIV-1 sensitive to VRC01. To inform future study design and dosing regimen selection of candidate bnAbs, we investigated the association of VRC01 serum concentration with HIV-1 acquisition using AMP trial data. METHODS: The case-control sample included 107 VRC01 recipients who acquired HIV-1 and 82 VRC01 recipients who remained without HIV-1 during the study. We measured VRC01 serum concentrations with a qualified pharmacokinetic (PK) Binding Antibody Multiplex Assay. We employed nonlinear mixed effects PK modelling to estimate daily-grid VRC01 concentrations. Cox regression models were used to assess the association of VRC01 concentration at exposure and baseline body weight, with the hazard of HIV-1 acquisition and prevention efficacy as a function of VRC01 concentration. We also compared fixed dosing vs. body weight-based dosing via simulations. FINDINGS: Estimated VRC01 concentrations in VRC01 recipients without HIV-1 were higher than those in VRC01 recipients who acquired HIV-1. Body weight was inversely associated with HIV-1 acquisition among both placebo and VRC01 recipients but did not modify the prevention efficacy of VRC01. VRC01 concentration was inversely correlated with HIV-1 acquisition, and positively correlated with prevention efficacy of VRC01. Simulation studies suggest that fixed dosing may be comparable to weight-based dosing in overall predicted prevention efficacy. INTERPRETATION: These findings suggest that bnAb serum concentration may be a useful marker for dosing regimen selection, and operationally efficient fixed dosing regimens could be considered for future trials of HIV-1 bnAbs. FUNDING: Was provided by the National Institutes of Health, National Institute of Allergy and Infectious Diseases (NIAID) (UM1 AI068614, to the HIV Vaccine Trials Network [HVTN]; UM1 A

Published

2023

2. High Asymptomatic Carriage With the Omicron Variant in South Africa.

Author

Garrett, Nigel, Garrett, Nigel, Tapley, Asa, Andriesen, Jessica, Seocharan, Ishen, Fisher, Leigh H, Bunts, Lisa, Espy, Nicole, Wallis, Carole L, Randhawa, April Kaur, Miner, Maurine D, Ketter, Nzeera, Yacovone, Margaret, Goga, Ameena, Huang, Yunda, Hural, John, Kotze, Philip, Bekker, Linda Gail, Gray, Glenda E, Corey, Lawrence, Ubuntu Study Team, Garrett, Nigel, Garrett, Nigel, Tapley, Asa, Andriesen, Jessica, Seocharan, Ishen, Fisher, Leigh H, Bunts, Lisa, Espy, Nicole, Wallis, Carole L, Randhawa, April Kaur, Miner, Maurine D, Ketter, Nzeera, Yacovone, Margaret, Goga, Ameena, Huang, Yunda, Hural, John, Kotze, Philip, Bekker, Linda Gail, Gray, Glenda E, Corey, Lawrence, and Ubuntu Study Team

Abstract

We report a 23% asymptomatic severe acute respiratory syndrome coronavirus 2 (SARS CoV-2) Omicron carriage rate in participants being enrolled into a clinical trial in South Africa, 15-fold higher than in trials before Omicron. We also found lower CD4 + T-cell counts in persons with human immunodeficiency virus (HIV) strongly correlated with increased odds of being SARS-CoV-2 polymerase chain reaction (PCR) positive.

Published

2022

3. Achieving intracellular cytokine staining assay concordance on two continents to assess HIV vaccine-induced T-cell responses.

Author

Dintwe, One, Dintwe, One, De Rosa, Stephen, Huang, Yunda, Flach, Britta, Manso, Bryce, Carter, Don, Omar, Faatima, Schwedhelm, Katharine, Yu, Chenchen, Lu, Huiyin, Morris, Daryl, Kee, Jia, Voillet, Valentin, Stirewalt, Michael, Hural, John, Moodie, Zoe, Frahm, Nicole, Cohen, Kristen, McElrath, M, Andersen-Nissen, Erica, Dintwe, One, Dintwe, One, De Rosa, Stephen, Huang, Yunda, Flach, Britta, Manso, Bryce, Carter, Don, Omar, Faatima, Schwedhelm, Katharine, Yu, Chenchen, Lu, Huiyin, Morris, Daryl, Kee, Jia, Voillet, Valentin, Stirewalt, Michael, Hural, John, Moodie, Zoe, Frahm, Nicole, Cohen, Kristen, McElrath, M, and Andersen-Nissen, Erica

Abstract

The HIV Vaccine Trials Network (HVTN) conducts clinical trials on 4 continents in pursuit of a safe and effective HIV vaccine. Cellular immune responses to vaccination that define vaccine immunogenicity and/or immune correlates of protection can be measured using multiparameter intracellular cytokine staining (ICS) assays. The HVTN cellular immunology laboratory, located in Seattle, WA, conducts ICS assays for vaccine trials according to Good Clinical Laboratory Practices (GCLP). In 2013, the HVTN established a second GCLP compliant cellular immunology laboratory in Cape Town, South Africa to assess vaccine immunogenicity for HVTN trials conducted on the African continent. To ensure ICS readouts in the 2 laboratories were directly comparable, we conducted concordance testing using PBMC from healthy controls and vaccine trial participants. Despite standardized procedures and instrumentation, shared quality control measures and quality assurance oversight, several factors impacted our ability to obtain close agreement in T-cell responses measured in the 2 laboratories. One of these was the type of fetal bovine serum (FBS) used in the assay, which impacted lymphocyte cell viability and background responses. In addition, the differences in supernatant removal technique also significantly affected our ability to detect positive responses to vaccine antigens. Standardization of these factors allowed us to achieve and maintain ICS assay concordance across the 2 laboratories over multiple years, accelerating our efforts to evaluate HIV vaccines. The insights gained in this process are valuable for assay transfer efforts by groups of investigators that need to directly compare data generated in different laboratories around the globe.

Published

2022

4. Antigenic competition in CD4+ T cell responses in a randomized, multicenter, double-blind clinical HIV vaccine trial.

Author

Kallas, Esper, Kallas, Esper, Grunenberg, Nicole, Yu, Chenchen, Manso, Bryce, Pantaleo, Giuseppe, Casapia, Martin, Baden, Lindsey, Valencia, Javier, Sobieszczyk, Magdalena, Van Tieu, Hong, Allen, Mary, Hural, John, Graham, Barney, Kublin, James, Gilbert, Peter, Corey, Lawrence, Goepfert, Paul, McElrath, M, Johnson, R, Huang, Yunda, Frahm, Nicole, Kallas, Esper, Kallas, Esper, Grunenberg, Nicole, Yu, Chenchen, Manso, Bryce, Pantaleo, Giuseppe, Casapia, Martin, Baden, Lindsey, Valencia, Javier, Sobieszczyk, Magdalena, Van Tieu, Hong, Allen, Mary, Hural, John, Graham, Barney, Kublin, James, Gilbert, Peter, Corey, Lawrence, Goepfert, Paul, McElrath, M, Johnson, R, Huang, Yunda, and Frahm, Nicole

Abstract

T cell responses have been implicated in reduced risk of HIV acquisition in uninfected persons and control of viral replication in HIV-infected individuals. HIV Gag-specific T cells have been predominantly associated with post-infection control, whereas Env antigens are the target for protective antibodies; therefore, inclusion of both antigens is common in HIV vaccine design. However, inclusion of multiple antigens may provoke antigenic competition, reducing the potential effectiveness of the vaccine. HVTN 084 was a randomized, multicenter, double-blind phase 1 trial to investigate whether adding Env to a Gag/Pol vaccine decreases the magnitude or breadth of Gag/Pol-specific T cell responses. Fifty volunteers each received one intramuscular injection of 1 × 1010 particle units (PU) of rAd5 Gag/Pol and EnvA/B/C (3:1:1:1 mixture) or 5 × 109 PU of rAd5 Gag/Pol. CD4+ T cell responses to Gag/Pol measured 4 weeks after vaccination by cytokine expression were significantly higher in the group vaccinated without Env, whereas CD8+ T cell responses did not differ significantly between the two groups. Mapping of individual epitopes revealed greater breadth of the Gag/Pol-specific T cell response in the absence of Env compared to Env coimmunization. Addition of an Env component to a Gag/Pol vaccine led to reduced Gag/Pol CD4+ T cell response rate and magnitude as well as reduced epitope breadth, confirming the presence of antigenic competition. Therefore, T cell-based vaccine strategies should aim at choosing a minimalist set of antigens to reduce interference of individual vaccine components with the induction of the maximally achievable immune response.

Published

2019