Your search keyword '"Nonhlanhla N. Mkhize"' showing total 55 results

1. Safety and pharmacokinetics of subcutaneous administration of broadly neutralizing anti-HIV-1 monoclonal antibodies (bNAbs), given to HIV-1 exposed, uninfected neonates and infants: study protocol for a phase I trial

Author

Ameena Goga, Trisha Ramraj, Logashvari Naidoo, Brodie Daniels, Masefetsane Matlou, Terusha Chetty, Reshmi Dassaye, Nobubelo K. Ngandu, Laura Galli, Tarylee Reddy, Ishen Seocharan, Qondeni Ndlangamandla, Qholokazi September, Nokwanda Ngcobo, Mayuri Reddy, Tamon Cafun-Naidoo, Kubashni Woeber, Nitesha Jeenarain, Rabia Imamdin, Keshnee Maharajh, Ashmintha Ramjeth, Thobile Bhengu, Emma Clarence, Philippe Van de Perre, Thorkild Tylleskär, Nicolas Nagot, Jean-Pierre Moles, Penny L. Moore, Nonhlanhla N. Mkhize, Lucio Gama, Stefania Dispinseri, Priscilla Biswas, Gabriella Scarlatti, and the PedMAb1 clinical trial team

Subjects

HIV, Broadly neutralizing antibody, Vertical transmission of HIV-1, Vertical transmission, Breastfeeding, Pre-exposure prophylaxis, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background The ambitious goal to eliminate new pediatric HIV infections by 2030 requires accelerated prevention strategies in high-risk settings such as South Africa. One approach could be pre-exposure prophylaxis (PrEP) with broadly neutralizing anti-HIV-1 monoclonal antibodies (bNAbs). The aim of our study is to define the optimal dose(s), the ideal combination(s) of bNAbs in terms of potency and breadth, and timing of subcutaneous (SC) administration(s) to prevent breast milk transmission of HIV. Methods Two bNAbs, CAP256V2LS and VRC07-523LS, will be assessed in a sequential and randomized phase I, single-site, single-blind, dose-finding trial. We aim to investigate the 28-day safety and pharmacokinetics (PK) profile of incrementally higher doses of these bNAbs in breastfeeding HIV-1 exposed born without HIV neonates alongside standard of care antiretroviral (ARV) medication to prevent (infants) or treat (mothers) HIV infection. The trial design includes 3 steps and 7 arms (1, 2, 3, 4, 5, 6 and 6b) with 8 infants in each arm. The first step will evaluate the safety and PK profile of the bNAbs when given alone as a single subcutaneous (SC) administration at increasing mg/kg body weight doses within 96 h of birth: arms 1, 2 and 3 at doses of 5, 10, and 20 mg/kg of CAP256V2LS, respectively; arms 4 and 5 at doses of 20 and 30 mg/kg of VRC07-523LS, respectively. Step two will evaluate the safety and PK profile of a combination of the two bNAbs administered SC at fixed doses within 96 h of birth. Step three will evaluate the safety and PK profile of the two bNAbs administered SC in combination at fixed doses, after 3 months. Arms 1 and 6 will follow sequential recruitment, whereas randomization will occur sequentially between arms (a) 2 & 4 and (b) 3 & 5. Before each randomization, a safety pause will allow review of safety data of the preceding arms. Discussion The results of this trial will guide further studies on bNAbs to prevent breast milk transmission of HIV. Protocol version Version 4.0 dated 15 March 2024. Trial registration Pan African Clinical Trial Registry (PACTR): PACTR202205715278722, 21 April 2022; South African National Clinical Trial Registry (SANCTR): DOH-27–062022-6058.

Published

2024

2. High monoclonal neutralization titers reduced breakthrough HIV-1 viral loads in the Antibody Mediated Prevention trials

Author

Daniel B. Reeves, Bryan T. Mayer, Allan C. deCamp, Yunda Huang, Bo Zhang, Lindsay N. Carpp, Craig A. Magaret, Michal Juraska, Peter B. Gilbert, David C. Montefiori, Katharine J. Bar, E. Fabian Cardozo-Ojeda, Joshua T. Schiffer, Raabya Rossenkhan, Paul Edlefsen, Lynn Morris, Nonhlanhla N. Mkhize, Carolyn Williamson, James I. Mullins, Kelly E. Seaton, Georgia D. Tomaras, Philip Andrew, Nyaradzo Mgodi, Julie E. Ledgerwood, Myron S. Cohen, Lawrence Corey, Logashvari Naidoo, Catherine Orrell, Paul A. Goepfert, Martin Casapia, Magdalena E. Sobieszczyk, Shelly T. Karuna, and Srilatha Edupuganti

Subjects

Science

Abstract

Abstract The Antibody Mediated Prevention (AMP) trials (NCT02716675 and NCT02568215) demonstrated that passive administration of the broadly neutralizing monoclonal antibody VRC01 could prevent some HIV-1 acquisition events. Here, we use mathematical modeling in a post hoc analysis to demonstrate that VRC01 influenced viral loads in AMP participants who acquired HIV. Instantaneous inhibitory potential (IIP), which integrates VRC01 serum concentration and VRC01 sensitivity of acquired viruses in terms of both IC50 and IC80, follows a dose-response relationship with first positive viral load (p = 0.03), which is particularly strong above a threshold of IIP = 1.6 (r = -0.6, p = 2e-4). Mathematical modeling reveals that VRC01 activity predicted from in vitro IC80s and serum VRC01 concentrations overestimates in vivo neutralization by 600-fold (95% CI: 300–1200). The trained model projects that even if future therapeutic HIV trials of combination monoclonal antibodies do not always prevent acquisition, reductions in viremia and reservoir size could be expected.

Published

2023

3. Author Correction: High monoclonal neutralization titers reduced breakthrough HIV-1 viral loads in the Antibody Mediated Prevention trials

Author

Daniel B. Reeves, Bryan T. Mayer, Allan C. deCamp, Yunda Huang, Bo Zhang, Lindsay N. Carpp, Craig A. Magaret, Michal Juraska, Peter B. Gilbert, David C. Montefiori, Katharine J. Bar, E. Fabian Cardozo-Ojeda, Joshua T. Schiffer, Raabya Rossenkhan, Paul Edlefsen, Lynn Morris, Nonhlanhla N. Mkhize, Carolyn Williamson, James I. Mullins, Kelly E. Seaton, Georgia D. Tomaras, Philip Andrew, Nyaradzo Mgodi, Julie E. Ledgerwood, Myron S. Cohen, Lawrence Corey, Logashvari Naidoo, Catherine Orrell, Paul A. Goepfert, Martin Casapia, Magdalena E. Sobieszczyk, Shelly T. Karuna, and Srilatha Edupuganti

Subjects

Science

Published

2024

4. Infection pre-Ad26.COV2.S-vaccination primes greater class switching and reduced CXCR5 expression by SARS-CoV-2-specific memory B cells

Author

Robert G. E. Krause, Thandeka Moyo-Gwete, Simone I. Richardson, Zanele Makhado, Nelia P. Manamela, Tandile Hermanus, Nonhlanhla N. Mkhize, Roanne Keeton, Ntombi Benede, Mathilda Mennen, Sango Skelem, Farina Karim, Khadija Khan, Catherine Riou, Ntobeko A. B. Ntusi, Ameena Goga, Glenda Gray, Willem Hanekom, Nigel Garrett, Linda-Gail Bekker, Andreas Groll, Alex Sigal, Penny L. Moore, Wendy A. Burgers, and Alasdair Leslie

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Neutralizing antibodies strongly correlate with protection for COVID-19 vaccines, but the corresponding memory B cells that form to protect against future infection are relatively understudied. Here we examine the effect of prior SARS-CoV-2 infection on the magnitude and phenotype of the memory B cell response to single dose Johnson and Johnson (Ad26.COV2.S) vaccination in South African health care workers. Participants were either naïve to SARS-CoV-2 or had been infected before vaccination. SARS-CoV-2-specific memory B-cells expand in response to Ad26.COV2.S and are maintained for the study duration (84 days) in all individuals. However, prior infection is associated with a greater frequency of these cells, a significant reduction in expression of the germinal center chemokine receptor CXCR5, and increased class switching. These B cell features correlated with neutralization and antibody-dependent cytotoxicity (ADCC) activity, and with the frequency of SARS-CoV-2 specific circulating T follicular helper cells (cTfh). Vaccination-induced effective neutralization of the D614G variant in both infected and naïve participants but boosted neutralizing antibodies against the Beta and Omicron variants only in participants with prior infection. In addition, the SARS-CoV-2 specific CD8+ T cell response correlated with increased memory B cell expression of the lung-homing receptor CXCR3, which was sustained in the previously infected group. Finally, although vaccination achieved equivalent B cell activation regardless of infection history, it was negatively impacted by age. These data show that phenotyping the response to vaccination can provide insight into the impact of prior infection on memory B cell homing, CSM, cTfh, and neutralization activity. These data can provide early signals to inform studies of vaccine boosting, durability, and co-morbidities.

Published

2023

5. Prediction of serum HIV-1 neutralization titers of VRC01 in HIV-uninfected Antibody Mediated Prevention (AMP) trial participants

Author

Yunda Huang, Lily Zhang, Amanda Eaton, Nonhlanhla N. Mkhize, Lindsay N. Carpp, Erika Rudnicki, Allan DeCamp, Michal Juraska, April Randhawa, Adrian McDermott, Julie Ledgerwood, Philip Andrew, Shelly Karuna, Srilatha Edupuganti, Nyaradzo Mgodi, Myron Cohen, Lawrence Corey, John Mascola, Peter B. Gilbert, Lynn Morris, and David C. Montefiori

Subjects

population pharmacokinetic modeling, pharmacokinetics/pharmacodynamics joint modeling, correlates analysis, monoclonal antibodies, hiv-1 prevention, broadly neutralizing antibody, breakthrough viruses, Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Abstract

VRC01 is being evaluated in the AMP efficacy trials, the first assessment of a passively administered broadly neutralizing monoclonal antibody (bnAb) for HIV-1 prevention. A key analysis will assess serum VRC01-mediated neutralization as a potential correlate of protection. To prepare for this analysis, we conducted a pilot study where we measured longitudinal VRC01 serum concentrations and serum VRC01-mediated neutralization in 47 and 31 HIV-1 uninfected AMP participants, respectively. We applied four different statistical approaches to predict serum VRC01-mediated neutralization titer against Env-pseudotyped viruses, including breakthrough viruses isolated from AMP placebo recipients who became HIV-1 infected during the trial, using VRC01 serum concentration and neutralization potency (IC50 or IC80) of the VRC01 clinical lot against the same virus. Approaches 3 and 4, which utilized pharmacokinetics/pharmacodynamics joint modeling of concentration and neutralization titer, generally performed the best or comparably to Approaches 1 and 2, which, respectively, utilized only measured and model-predicted concentration. For prediction of ID80 titers against breakthrough viruses, Approaches 1 and 2 rendered comparable performance to Approaches 3 and 4, and could be reasonable approaches to adopt in practice as they entail reduced assay cost and less complicated statistical analysis. Our results may be applied to future studies of other bnAbs and bnAb combinations to maximize resource efficiency in serum neutralization titer measurement.

Published

2022

6. Effect of HIV Envelope Vaccination on the Subsequent Antibody Response to HIV Infection

Author

Zanele Ditse, Nonhlanhla N. Mkhize, Michael Yin, Michael Keefer, David C. Montefiori, Georgia D. Tomaras, Gavin Churchyard, Kenneth H. Mayer, Shelly Karuna, Cecilia Morgan, Linda-Gail Bekker, Koleka Mlisana, Glenda Gray, Zoe Moodie, Peter Gilbert, Penny L. Moore, Carolyn Williamson, and Lynn Morris

Subjects

HIV vaccines, HIV breakthrough infections, HIV-specific binding antibodies, broadly neutralizing antibodies, DNA/MVA vaccines, rAd5, Microbiology, QR1-502

Abstract

ABSTRACT Analysis of breakthrough HIV-1 infections could elucidate whether prior vaccination primes relevant immune responses. Here, we measured HIV-specific antibody responses in 14 South African volunteers who acquired HIV infection after participating in phase 1/2 trials of envelope-containing immunogens. Serum samples were collected annually following HIV-1 infection from participants in trials HVTN 073 (subtype C, DNA/MVA, phase 1 trial, n = 1), HVTN 086 (subtype C, DNA/MVA/gp140 protein, phase 1 trial, n = 2), and HVTN 204 (multisubtype, DNA/adenovirus serotype 5 [Ad5], phase 2 trial, n = 7) and 4 placebo recipients. Binding and neutralizing antibody responses to Env proteins and peptides were determined pre- and post-HIV infection using an enzyme-linked immunosorbent assay and the TZM-bl cell neutralization assay, respectively. HIV-infected South African individuals served as unvaccinated controls. Binding antibodies to gp41, V3, V2, the membrane-proximal external region (MPER), and the CD4 binding site were detected from the first year of HIV-1 subtype C infection, and the levels were similar in vaccinated and placebo recipients. Neutralizing antibody responses against tier 1A viruses were detected in all participants, with the highest titers being to a subtype C virus, MW965.26. No responses were observed just prior to infection, indicating that vaccine-primed HIV-specific antibodies had waned. Sporadic neutralization activity against tier 2 isolates was observed after 2 to 3 years of HIV infection, but these responses were similar in the vaccinated and placebo groups as well as the unvaccinated controls. Our data suggest that prior vaccination with these immunogens did not alter the antibody responses to HIV-1 infection, nor did it accelerate the development of HIV neutralization breadth. IMPORTANCE There is a wealth of information on HIV-specific vaccine-induced immune responses among HIV-uninfected participants; however, data on immune responses among participants who acquire HIV after vaccination are limited. Here we show that HIV-specific binding antibody responses in individuals with breakthrough HIV infections were not affected by prior vaccination with HIV envelope-containing immunogens. We also found that these vectored vaccines did not prime tier 2 virus-neutralizing antibody responses, which are thought to be required for prevention against HIV acquisition, or accelerate the development of neutralization breadth. Although this study is limited, such studies can provide insights into whether vaccine-elicited antibody responses are boosted by HIV infection to acquire broader neutralizing activity, which may help to identify antigens relevant to the design of more effective vaccines.

Published

2020

7. V2-Directed Vaccine-like Antibodies from HIV-1 Infection Identify an Additional K169-Binding Light Chain Motif with Broad ADCC Activity

Author

Charmaine van Eeden, Constantinos Kurt Wibmer, Cathrine Scheepers, Simone I. Richardson, Molati Nonyane, Bronwen Lambson, Nonhlanhla N. Mkhize, Balakrishnan Vijayakumar, Zizhang Sheng, Sherry Stanfield-Oakley, Jinal N. Bhiman, Valerie Bekker, Tandile Hermanus, Batsirai Mabvakure, Arshad Ismail, M. Anthony Moody, Kevin Wiehe, Nigel Garrett, Salim Abdool Karim, Heini Dirr, Manuel A. Fernandes, Yasien Sayed, Lawrence Shapiro, Guido Ferrari, Barton F. Haynes, Penny L. Moore, and Lynn Morris

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Antibodies that bind residue K169 in the V2 region of the HIV-1 envelope correlated with reduced risk of infection in the RV144 vaccine trial but were restricted to two ED-motif-encoding light chain genes. Here, we identify an HIV-infected donor with high-titer V2 peptide-binding antibodies and isolate two antibody lineages (CAP228-16H/19F and CAP228-3D) that mediate potent antibody-dependent cell-mediated cytotoxicity (ADCC). Both lineages use the IGHV5-51 heavy chain germline gene, similar to the RV144 antibody CH58, but one lineage (CAP228-16H/19F) uses a light chain without the ED motif. A cocrystal structure of CAP228-16H bound to a V2 peptide identified a IGLV3-21 gene-encoded DDxD motif that is used to bind K169, with a mechanism that allows CAP228-16H to recognize more globally relevant V2 immunotypes. Overall, these data further our understanding of the development of cross-reactive, V2-binding, antiviral antibodies and effectively expand the human light chain repertoire able to respond to RV144-like immunogens. : V2-directed antibodies from the RV144 vaccine trial correlated with reduced HIV-1 infection risk but exhibited restricted light chain gene usage. Here, van Eeden et al. isolate similar antibodies from an HIV-1-infected individual and identify a third V2-reactive light chain gene, increasing the antibody repertoire potentially elicited by vaccination. Keywords: HIV, V2 antibodies, K169, V2 structure, ED motif, CAP228, CH58, antibody evolution, ADCC, RV144 vaccine response

Published

2018

8. Safety and pharmacokinetics of escalating doses of neutralising monoclonal antibody CAP256V2LS administered with and without VRC07-523LS in HIV-negative women in South Africa (CAPRISA 012B): a phase 1, dose-escalation, randomised controlled trial

Author

Sharana Mahomed, Nigel Garrett, Edmund V Capparelli, Farzana Osman, Nonhlanhla N Mkhize, Ishana Harkoo, Tanuja N Gengiah, Leila E Mansoor, Cheryl Baxter, Derseree Archary, Nonhlanhla Yende-Zuma, Natasha Samsunder, Kevin Carlton, Sandeep Narpala, Adrian B McDermott, Nicole A Doria-Rose, Penny L Moore, Lynn Morris, Quarraisha Abdool Karim, John R Mascola, and Salim S Abdool Karim

Subjects

Infectious Diseases, Epidemiology, Virology, Immunology

Published

2023

9. Safety and Pharmacokinetics of Monoclonal Antibodies VRC07-523LS and PGT121 Administered Subcutaneously for Human Immunodeficiency Virus Prevention

Author

Sharana Mahomed, Nigel Garrett, Edmund V Capparelli, Farzana Osman, Ishana Harkoo, Nonhlanhla Yende-Zuma, Tanuja N Gengiah, Derseree Archary, Natasha Samsunder, Cheryl Baxter, Nonhlanhla N Mkhize, Tandile Modise, Kevin Carlton, Adrian McDermott, Penny L Moore, Quarraisha Abdool Karim, Dan H Barouch, Patricia E Fast, John R Mascola, Julie E Ledgerwood, Lynn Morris, and Salim S Abdool Karim

Subjects

Antineoplastic Agents, Immunological, Infectious Diseases, Immunization, Passive, Antibodies, Monoclonal, HIV, Humans, Immunology and Allergy, Female, HIV Infections, HIV Antibodies, Antibodies, Neutralizing

Abstract

Background Effective, long-acting prevention approaches are needed to reduce human immunodeficiency virus (HIV) incidence. We evaluated the safety and pharmacokinetics of VRC07-523LS and PGT121 administered subcutaneously alone and in combination as passive immunization for young women in South Africa. Methods CAPRISA 012A was a randomized, double-blinded, placebo-controlled, dose-escalation phase 1 trial. We enrolled 45 HIV-negative women into 9 groups and assessed safety, tolerability, pharmacokinetics, neutralization activity, and antidrug antibody levels. Pharmacokinetic modeling was conducted to predict steady-state concentrations for 12- and 24-weekly dosing intervals. Results VRC07-523LS and PGT121, administered subcutaneously, were safe and well tolerated. Most common reactogenicity events were injection site tenderness and headaches. Nine product-related adverse events were mild and transient. Median VRC07-523LS concentrations after 20 mg/kg doses were 9.65 μg/mL and 3.86 μg/mL at 16 and 24 weeks. The median week 8 concentration after the 10 mg/kg PGT121 dose was 8.26 μg/mL. Modeling of PGT121 at 20 mg/kg showed median concentrations of 1.37 μg/mL and 0.22 μg/mL at 16 and 24 weeks. Half-lives of VRC07-523LS and PGT121 were 29 and 20 days. Both antibodies retained neutralizing activity postadministration and no antidrug antibodies were detected. Conclusions Subcutaneous administration of VRC07-523LS in combination with optimized versions of PGT121 or other antibodies should be further assessed for HIV prevention.

Published

2022

10. Shared N417-Dependent Epitope on the SARS-CoV-2 Omicron, Beta, and Delta Plus Variants

Author

Thandeka Moyo-Gwete, Mashudu Madzivhandila, Nonhlanhla N Mkhize, Prudence Kgagudi, Frances Ayres, Bronwen E Lambson, Nelia P Manamela, Simone I Richardson, Zanele Makhado, Mieke A van der Mescht, Zelda de Beer, Talita Roma de Villiers, Wendy A Burgers, Ntobeko A B Ntusi, Theresa Rossouw, Veronica Ueckermann, Michael T Boswell, and Penny L Moore

Subjects

SARS-CoV-2, Immunology, Antibodies, Monoclonal, COVID-19, Cross Reactions, Antibodies, Viral, Antibodies, Neutralizing, Microbiology, Epitopes, Neutralization Tests, Virology, Insect Science, Spike Glycoprotein, Coronavirus, Humans, Immune Evasion

Abstract

As SARS-CoV-2 continues to evolve, several variants of concern (VOCs) have arisen which are defined by multiple mutations in their spike proteins. These VOCs have shown variable escape from antibody responses, and have been shown to trigger qualitatively different antibody responses during infection. By studying plasma from individuals infected with either the original D614G, Beta or Delta variants, we show that the Beta and Delta variants elicit antibody responses that are overall more cross-reactive than those triggered by D614G. Patterns of cross-reactivity varied, and the Beta and Delta variants did not elicit cross-reactive responses to each other. However, Beta-elicited plasma was highly cross-reactive against Delta plus (Delta+) which differs from Delta by a single K417N mutation in the receptor binding domain, suggesting the plasma response targets the N417 residue. To probe this further, we isolated monoclonal antibodies from a Beta-infected individual with plasma responses against Beta, Delta+ and Omicron, which all possess the N417 residue. We isolated a N417-dependent antibody, 084-7D, which showed similar neutralization breadth to the plasma. The 084-7D mAb utilized the IGHV3-23*01 germline gene and had similar somatic hypermutations compared to previously described public antibodies which target the 417 residue. Thus, we have identified a novel antibody which targets a shared epitope found on three distinct VOCs, enabling their cross-neutralization. Understanding antibodies targetting escape mutations such as K417N, which repeatedly emerge through convergent evolution in SARS-CoV-2 variants, may aid in the development of next-generation antibody therapeutics and vaccines.ImportanceThe evolution of SARS-CoV-2 has resulted in variants of concern (VOCs) with distinct spike mutations conferring varying immune escape profiles. These variable mutations also influence the cross-reactivity of the antibody response mounted by individuals infected with each of these variants. This study sought to understand the antibody responses elicited by different SARS-CoV-2 variants, and to define shared epitopes. We show that Beta and Delta infection resulted in antibody responses that were more cross-reactive compared to the original D614G variant, but each with differing patterns of cross-reactivity. We further isolated an antibody from Beta infection, which targeted the N417 site, enabling cross-neutralization of Beta, Delta+ and Omicron, all of which possess this residue. The discovery of antibodies which target escape mutations common to multiple variants highlights conserved epitopes to target in future vaccines and therapeutics.

Published

2022

11. Neutralization titer biomarker for antibody-mediated prevention of HIV-1 acquisition

Author

Peter B. Gilbert, Yunda Huang, Allan C. deCamp, Shelly Karuna, Yuanyuan Zhang, Craig A. Magaret, Elena E. Giorgi, Bette Korber, Paul T. Edlefsen, Raabya Rossenkhan, Michal Juraska, Erika Rudnicki, Nidhi Kochar, Ying Huang, Lindsay N. Carpp, Dan H. Barouch, Nonhlanhla N. Mkhize, Tandile Hermanus, Prudence Kgagudi, Valerie Bekker, Haajira Kaldine, Rutendo E. Mapengo, Amanda Eaton, Elize Domin, Carley West, Wenhong Feng, Haili Tang, Kelly E. Seaton, Jack Heptinstall, Caroline Brackett, Kelvin Chiong, Georgia D. Tomaras, Philip Andrew, Bryan T. Mayer, Daniel B. Reeves, Magdalena E. Sobieszczyk, Nigel Garrett, Jorge Sanchez, Cynthia Gay, Joseph Makhema, Carolyn Williamson, James I. Mullins, John Hural, Myron S. Cohen, Lawrence Corey, David C. Montefiori, and Lynn Morris

Subjects

HIV-1, Animals, Humans, HIV Infections, General Medicine, HIV Antibodies, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology, Adenosine Monophosphate, Biomarkers, Broadly Neutralizing Antibodies

Abstract

The Antibody Mediated Prevention trials showed that the broadly neutralizing antibody (bnAb) VRC01 prevented acquisition of human immunodeficiency virus-1 (HIV-1) sensitive to VRC01. Using AMP trial data, here we show that the predicted serum neutralization 80% inhibitory dilution titer (PT80) biomarker—which quantifies the neutralization potency of antibodies in an individual’s serum against an HIV-1 isolate—can be used to predict HIV-1 prevention efficacy. Similar to the results of nonhuman primate studies, an average PT80 of 200 (meaning a bnAb concentration 200-fold higher than that required to reduce infection by 80% in vitro) against a population of probable exposing viruses was estimated to be required for 90% prevention efficacy against acquisition of these viruses. Based on this result, we suggest that the goal of sustained PT80 >200 against 90% of circulating viruses can be achieved by promising bnAb regimens engineered for long half-lives. We propose the PT80 biomarker as a surrogate endpoint for evaluation of bnAb regimens, and as a tool for benchmarking candidate bnAb-inducing vaccines.

Published

2021

12. Prediction of serum HIV-1 neutralization titers of VRC01 in HIV-uninfected Antibody Mediated Prevention (AMP) trial participants

Author

Lindsay N. Carpp, Lawrence Corey, Allan C. deCamp, John R. Mascola, Adrian B. McDermott, Nyaradzo Mgodi, Peter B. Gilbert, Lynn Morris, Michal Juraska, Amanda Eaton, Nonhlanhla N. Mkhize, Yunda Huang, Erika Rudnicki, Srilatha Edupuganti, David C. Montefiori, Myron S. Cohen, Julie E. Ledgerwood, Lily Zhang, Shelly Karuna, Philip Andrew, and April K. Randhawa

Subjects

medicine.drug_class, Immunology, HIV Infections, Pilot Projects, HIV Antibodies, Monoclonal antibody, Neutralization, Virus, Pharmacokinetics, HIV Seropositivity, medicine, Immunology and Allergy, Potency, Humans, Pharmacology, biology, business.industry, Antibodies, Monoclonal, Antibodies, Neutralizing, Adenosine Monophosphate, Titer, Pharmacodynamics, biology.protein, HIV-1, Antibody, business, Broadly Neutralizing Antibodies

Abstract

VRC01 is being evaluated in the AMP efficacy trials, the first assessment of a passively administered broadly neutralizing monoclonal antibody (bnAb) for HIV-1 prevention. A key analysis will assess serum VRC01-mediated neutralization as a potential correlate of protection. To prepare for this analysis, we conducted a pilot study where we measured longitudinal VRC01 serum concentrations and serum VRC01-mediated neutralization in 47 and 31 HIV-1 uninfected AMP participants, respectively. We applied four different statistical approaches to predict serum VRC01-mediated neutralization titer against Env-pseudotyped viruses, including breakthrough viruses isolated from AMP placebo recipients who became HIV-1 infected during the trial, using VRC01 serum concentration and neutralization potency (IC50 or IC80) of the VRC01 clinical lot against the same virus. Approaches 3 and 4, which utilized pharmacokinetics/pharmacodynamics joint modeling of concentration and neutralization titer, generally performed the best or comparably to Approaches 1 and 2, which, respectively, utilized only measured and model-predicted concentration. For prediction of ID80 titers against breakthrough viruses, Approaches 1 and 2 rendered comparable performance to Approaches 3 and 4, and could be reasonable approaches to adopt in practice as they entail reduced assay cost and less complicated statistical analysis. Our results may be applied to future studies of other bnAbs and bnAb combinations to maximize resource efficiency in serum neutralization titer measurement.

Published

2021

13. Geografiese ligging beïnvloed vaginale mikrobiese profiele in Suid-Afrikaanse vroue

Author

Nonhlanhla N. Mkhize, Katie Lennard, Enock Havyarimana, Anna K. Blakney, David A. Lewis, Shameem Z. Jaumdally, Heather B. Jaspan, Glenda Gray, Smritee Dabee, Jo-Ann S. Passmore, Nicola Mulder, Linda-Gail Bekker, Gerrit Botha, and Shaun L. Barnabas

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 030106 microbiology, Biology

Abstract

Vroue van Afrika-afkoms is meer vatbaar vir bakteriële vaginose (BV) in vergelyking met Europese vroue. Beide mikrobiese diversiteit (soos met BV) sowel as spesifieke bakteriële taksa speel ‘n rol in seksuele en reproduktiewe gesondheid insluitende MIV vatbaarheid. Die moontlike rol van geografi ese ligging en etnisiteit op die verhouding tussen mikrobiese samestelling en seskuele en reproduktiewe gesondheid bly egter onbekend. In hierdie studie vergelyk ons dus die vaginale mikrobiota van 16–22-jarige swart, HIV-negatiewe Suid-Afrikaanse vroue van twee geografies-uiteenlopende liggings, beide lae-inkomste, hoë bevolkingsdigtheidsgemeenskappe, een in Kaapstad, en een in Johannesburg. Vaginale mikrobiese profiele is bepaal met behulp van 16S rRNS volgordebepaling van laterale muur deppers. Ons pas permutasie variansieanalise (PERMANOVA) toe en vind statisties betekenisvolle assosiasies tussen vaginale mikrobiese samestelling en geografiese ligging (p=0.02), asook met liggaamsmassa-indeks (LMI) (p=0.015) en menslike papilloomvirus (MPV) risikotipe (p=0.005), maar nie met die voorkoms van een of meer seksueel-oordraagbare infeksies (SOI’s) (p=0.053) of met hormonale kontrasepsie verbruik nie. (p=0.4) Geografiese ligging was ‘n statisties betekenisvolle determinant van mikrobiese samestelling, ongeag verskille in LMI, SOI status en MPV-risiko tipes tussen Kaapstad en Johannesburg vroue. Geografiese ligging, LMI en MPV-risiko verduidelik gesamentlik 10% van die variansie in mikrobiese samestelling, met ‘n groot persentasie van onbekende oorsprong. Verskeie taksa het statisties betekenisvol verskil in terme van frekwensie of relatiewe vlakke van voorkoms tussen die geografiese liggings. Ons resultate stel voor dat MIV profi laktiese metodes wat die vaginale

Published

2019

14. Measuring the ability of HIV-specific antibodies to mediate trogocytosis

Author

Nonhlanhla N. Mkhize, Simone I. Richardson, Carol Crowther, and Lynn Morris

Subjects

CD4-Positive T-Lymphocytes, Male, 0301 basic medicine, Trogocytosis, THP-1 Cells, Phagocytosis, Immunology, HIV Infections, HIV Antibodies, Epitope, Flow cytometry, Epitopes, 03 medical and health sciences, medicine, Humans, Immunology and Allergy, Receptor, biology, medicine.diagnostic_test, Chemistry, Effector, Receptors, IgG, Antibody-Dependent Cell Cytotoxicity, Flow Cytometry, Antibodies, Neutralizing, 030104 developmental biology, Membrane protein, HIV-1, biology.protein, Female, Antibody

Abstract

Antibody Fc effector functions contribute to HIV control and have been implicated in the partial efficacy seen in the RV144 vaccine trial. Fc-mediated trogocytosis has been previously described for anti-cancer antibodies and results in the removal of membrane fragments from target cells. Here we developed a flow cytometry-based assay which measures the transfer of membrane fragments from a gp120-coated CD4+ lymphocytic cell line (CEM.NKR-CCR5 cells stained with a membrane dye PKH26) to monocytic cells (THP-1 cells stained with CFSE). We showed that this transfer occurred rapidly, within 1 h, and was mediated through engagement of the FcγRIIa/b receptors on the THP-1 cells. HIV-specific IgG as well as gp120 and CD4 could be detected on the surface of THP-1 cells in a process that we demonstrated was distinct from phagocytosis. Furthermore, while the THP-1 effector cells remained intact following the receipt of new membrane proteins, the viability of the target CEM.NKR-CCR5 cells decreased over time. Analysis of HIV-specific plasma revealed that antibodies with trogocytic activity were common in acute and chronic HIV infection but were higher in individuals with broadly neutralizing antibody responses We also examined trogocytosis mediated by broadly neutralizing antibodies (bNAbs) targeting multiple epitopes on the BG505.SOSIP.664 trimer and show that levels of binding correlated with the trogocytosis score. Overall, our data describe a new antiviral Fc effector function mediated by HIV-specific antibodies that could be harnessed for vaccination and cure strategies.

Published

2018

15. V2-Directed Vaccine-like Antibodies from HIV-1 Infection Identify an Additional K169-Binding Light Chain Motif with Broad ADCC Activity

Author

Arshad Ismail, Barton F. Haynes, Tandile Hermanus, Molati Nonyane, Lynn Morris, M. Anthony Moody, Heini W. Dirr, Valerie Bekker, Constantinos Kurt Wibmer, Salim S. Abdool Karim, Yasien Sayed, Balakrishnan Vijayakumar, Sherry Stanfield-Oakley, Nonhlanhla N. Mkhize, Lawrence Shapiro, Jinal N. Bhiman, Nigel Garrett, Batsirai Mabvakure, Zizhang Sheng, Penny L. Moore, Bronwen E. Lambson, Simone I. Richardson, Manuel A. Fernandes, Kevin Wiehe, Guido Ferrari, Charmaine. van Eeden, and Cathrine Scheepers

Subjects

0301 basic medicine, Models, Molecular, HIV Infections, Biology, HIV Antibodies, HIV Envelope Protein gp120, Immunoglobulin light chain, General Biochemistry, Genetics and Molecular Biology, Germline, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Humans, 030212 general & internal medicine, Amino Acid Sequence, Cytotoxicity, Gene, lcsh:QH301-705.5, Alleles, Antibody-dependent cell-mediated cytotoxicity, AIDS Vaccines, Lysine, Vaccine trial, Antibody-Dependent Cell Cytotoxicity, Virology, Tissue Donors, 3. Good health, 030104 developmental biology, lcsh:Biology (General), biology.protein, Immunoglobulin Light Chains, Antibody, Peptides, Protein Binding

Abstract

SUMMARY Antibodies that bind residue K169 in the V2 region of the HIV-1 envelope correlated with reduced risk of infection in the RV144 vaccine trial but were restricted to two ED-motif-encoding light chain genes. Here, we identify an HIV-infected donor with high-titer V2 peptide-binding antibodies and isolate two antibody lineages (CAP228-16H/19F and CAP228–3D) that mediate potent antibody-dependent cell-mediated cytotoxicity (ADCC). Both lineages use the IGHV5–51 heavy chain germline gene, similar to the RV144 antibody CH58, but one lineage (CAP228-16H/19F) uses a light chain without the ED motif. A cocrystal structure of CAP228-16H bound to a V2 peptide identified a IGLV3–21 gene-encoded DDxD motif that is used to bind K169, with a mechanism that allows CAP228-16H to recognize more globally relevant V2 immunotypes. Overall, these data further our understanding of the development of cross-reactive, V2-binding, antiviral antibodies and effectively expand the human light chain repertoire able to respond to RV144-like immunogens., In Brief V2-directed antibodies from the RV144 vaccine trial correlated with reduced HIV-1 infection risk but exhibited restricted light chain gene usage. Here, van Eeden et al. isolate similar antibodies from an HIV-1-infected individual and identify a third V2-reactive light chain gene, increasing the antibody repertoire potentially elicited by vaccination., Graphical Abstract

Published

2018

16. Initiation of Antiretroviral Therapy Differentially Influences Genital and Systemic Immune Activation in HIV-Infected Women

Author

Jo-Ann S. Passmore, Nonhlanhla N. Mkhize, Smritee Dabee, David A. Lewis, Heather B. Jaspan, and Pamela P. Gumbi

Subjects

CD4-Positive T-Lymphocytes, T cell, Immunology, Human immunodeficiency virus (HIV), Viremia, HIV Infections, medicine.disease_cause, Virology, Hiv infected, Antiretroviral Therapy, Highly Active, Medicine, Humans, Sex organ, business.industry, virus diseases, Genitalia, Female, Viral Load, medicine.disease, Antiretroviral therapy, Infectious Diseases, medicine.anatomical_structure, Cross-Sectional Studies, Quality of Life, Female, business, Immune activation

Abstract

Antiretroviral therapy (ART) has significantly improved the quality of life of HIV-infected individuals: reducing plasma viremia, restoring CD4+ T cell numbers, and correcting imbalances in blood m...

Published

2020

17. Effect of HIV Envelope Vaccination on the Subsequent Antibody Response to HIV Infection

Author

Carolyn Williamson, Kenneth H. Mayer, Glenda Gray, Zoe Moodie, Koleka Mlisana, Nonhlanhla N. Mkhize, Shelly Karuna, Linda-Gail Bekker, Penny L. Moore, Peter B. Gilbert, Gavin J. Churchyard, Georgia D. Tomaras, Cecilia Morgan, Michael Yin, David C. Montefiori, Michael C. Keefer, Lynn Morris, and Zanele Ditse

Subjects

Male, 0301 basic medicine, HIV breakthrough infections, lcsh:QR1-502, HIV Infections, HIV Antibodies, lcsh:Microbiology, Neutralization, 0302 clinical medicine, Medicine, Neutralizing antibody, AIDS Vaccines, biology, env Gene Products, Human Immunodeficiency Virus, virus diseases, Middle Aged, Viral Load, QR1-502, HIV Envelope Protein gp41, rAd5, 3. Good health, Vaccination, 030220 oncology & carcinogenesis, Female, Antibody, Research Article, Adult, Enzyme-Linked Immunosorbent Assay, Gp41, Microbiology, Virus, Young Adult, 03 medical and health sciences, Immune system, Antigen, Neutralization Tests, Humans, HIV-specific binding antibodies, Molecular Biology, business.industry, broadly neutralizing antibodies, HIV vaccines, Therapeutics and Prevention, Antibodies, Neutralizing, Virology, HIV-1 envelope, binding antibody epitopes, 030104 developmental biology, Antibody Formation, HIV-1, biology.protein, DNA/MVA vaccines, business

Abstract

There is a wealth of information on HIV-specific vaccine-induced immune responses among HIV-uninfected participants; however, data on immune responses among participants who acquire HIV after vaccination are limited. Here we show that HIV-specific binding antibody responses in individuals with breakthrough HIV infections were not affected by prior vaccination with HIV envelope-containing immunogens. We also found that these vectored vaccines did not prime tier 2 virus-neutralizing antibody responses, which are thought to be required for prevention against HIV acquisition, or accelerate the development of neutralization breadth. Although this study is limited, such studies can provide insights into whether vaccine-elicited antibody responses are boosted by HIV infection to acquire broader neutralizing activity, which may help to identify antigens relevant to the design of more effective vaccines., Analysis of breakthrough HIV-1 infections could elucidate whether prior vaccination primes relevant immune responses. Here, we measured HIV-specific antibody responses in 14 South African volunteers who acquired HIV infection after participating in phase 1/2 trials of envelope-containing immunogens. Serum samples were collected annually following HIV-1 infection from participants in trials HVTN 073 (subtype C, DNA/MVA, phase 1 trial, n = 1), HVTN 086 (subtype C, DNA/MVA/gp140 protein, phase 1 trial, n = 2), and HVTN 204 (multisubtype, DNA/adenovirus serotype 5 [Ad5], phase 2 trial, n = 7) and 4 placebo recipients. Binding and neutralizing antibody responses to Env proteins and peptides were determined pre- and post-HIV infection using an enzyme-linked immunosorbent assay and the TZM-bl cell neutralization assay, respectively. HIV-infected South African individuals served as unvaccinated controls. Binding antibodies to gp41, V3, V2, the membrane-proximal external region (MPER), and the CD4 binding site were detected from the first year of HIV-1 subtype C infection, and the levels were similar in vaccinated and placebo recipients. Neutralizing antibody responses against tier 1A viruses were detected in all participants, with the highest titers being to a subtype C virus, MW965.26. No responses were observed just prior to infection, indicating that vaccine-primed HIV-specific antibodies had waned. Sporadic neutralization activity against tier 2 isolates was observed after 2 to 3 years of HIV infection, but these responses were similar in the vaccinated and placebo groups as well as the unvaccinated controls. Our data suggest that prior vaccination with these immunogens did not alter the antibody responses to HIV-1 infection, nor did it accelerate the development of HIV neutralization breadth. IMPORTANCE There is a wealth of information on HIV-specific vaccine-induced immune responses among HIV-uninfected participants; however, data on immune responses among participants who acquire HIV after vaccination are limited. Here we show that HIV-specific binding antibody responses in individuals with breakthrough HIV infections were not affected by prior vaccination with HIV envelope-containing immunogens. We also found that these vectored vaccines did not prime tier 2 virus-neutralizing antibody responses, which are thought to be required for prevention against HIV acquisition, or accelerate the development of neutralization breadth. Although this study is limited, such studies can provide insights into whether vaccine-elicited antibody responses are boosted by HIV infection to acquire broader neutralizing activity, which may help to identify antigens relevant to the design of more effective vaccines.

Published

2020

18. 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

19. Converging epidemics of sexually transmitted infections and bacterial vaginosis in southern African female adolescents at risk of HIV

Author

Clive M. Gray, Heather B. Jaspan, Thomas J. Hope, Shameem Z. Jaumdally, Francesca Chiodi, Anna-Lise Williamson, Janan Dietrich, Venessa Maseko, David A. Lewis, Nonhlanhla N. Mkhize, Linda-Gail Bekker, Lindi Masson, Hoyam Gamieldien, Smritee Dabee, Zizipho Z. A. Mbulawa, Glenda Gray, Jo-Ann S. Passmore, Etienne E. Müller, and Shaun L. Barnabas

Subjects

0301 basic medicine, medicine.medical_specialty, Adolescent, Sexually Transmitted Diseases, Prevalence, Human immunodeficiency virus (HIV), HIV Infections, Dermatology, urologic and male genital diseases, Hiv risk, medicine.disease_cause, South Africa, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Vaginal disease, Risk groups, HIV Seronegativity, Poverty Areas, Internal medicine, Epidemiology, Humans, Medicine, Pharmacology (medical), 030212 general & internal medicine, Epidemics, business.industry, Public Health, Environmental and Occupational Health, virus diseases, Vaginosis, Bacterial, medicine.disease, female genital diseases and pregnancy complications, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Vagina, Female, Bacterial vaginosis, business

Abstract

Adolescents in Africa are at high risk for HIV infection, other sexually transmitted infections (STIs) and bacterial vaginosis (BV). Since behavior and burden of STIs/BV may influence HIV risk, behavioral risk factors and prevalence of STIs/BV were compared in HIV-seronegative adolescent females (n = 298; 16–22 years) from two South African communities (Soweto and Cape Town). STIs ( Chlamydia trachomatis, Neisseria gonorrhoeae, Trichomonas vaginalis, Mycoplasma genitalium, herpes simplex virus (HSV)-1, HSV-2, Treponema pallidum, and Haemophilus ducreyi) were detected by multiplex polymerase chain reaction, human papillomavirus (HPV) by Roche Linear Array, and BV by Nugent scoring. Rates of BV (Nugent ≥7; 46.6%) and HPV (66.8%) were high in both communities. Prevalence of C. trachomatis and N. gonorrhoeae were >2-fold higher in Cape Town than Soweto (Chlamydia: 42% [62/149] versus 18% [26/148], p 70% of young women with treatable conditions that could enhance HIV risk would have been missed because they lacked symptoms associated with syndromic management.

Published

2017

20. Antibody and cellular responses to HIV vaccine regimens with DNA plasmid as compared with ALVAC priming: An analysis of two randomized controlled trials

Author

Allan C. deCamp, Mary Allen, James G. Kublin, M. Juliana McElrath, Mina C. Hosseinipour, Craig Innes, Zoe Moodie, Giuseppe Pantaleo, Jack Heptinstall, Chenchen Yu, Nonhlanhla N. Mkhize, Nicole Frahm, Peter B. Gilbert, Erica Andersen-Nissen, Maurine D. Miner, Linda-Gail Bekker, Fatima Laher, Sarita Naidoo, Glenda Gray, Kristen W. Cohen, Julia Hutter, Hvtn trial teams, Philipp Mann, Lucas Maganga, David C. Montefiori, Lynn Morris, Ralf Wagner, One Dintwe, Georgia D. Tomaras, Nicole L. Yates, Nicole Grunenberg, Stephen R. Walsh, and Michael E Herce

Subjects

Male, HIV Antigens, Physiology, Molecular biology, medicine.medical_treatment, MF59, Antibody Response, HIV Infections, 030204 cardiovascular system & hematology, HIV Antibodies, Gastroenterology, Biochemistry, White Blood Cells, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine and Health Sciences, 030212 general & internal medicine, HIV vaccine, Immune Response, AIDS Vaccines, Vaccines, Immune System Proteins, T Cells, Immunogenicity, Vaccination, General Medicine, Infectious Diseases, Medicine, Female, Cellular Types, Adjuvant, Plasmids, Research Article, Adult, medicine.medical_specialty, Infectious Disease Control, Immune Cells, Genetic Vectors, Immunology, DNA construction, Microbiology, Antibodies, 03 medical and health sciences, Young Adult, Antigen, Double-Blind Method, Internal medicine, Virology, medicine, Humans, Antigens, Blood Cells, business.industry, Viral vaccines, HIV vaccines, Biology and Life Sciences, Proteins, DNA, Cell Biology, Antibodies, Neutralizing, Research and analysis methods, Regimen, Molecular biology techniques, Antibody Formation, Plasmid Construction, HIV-1, business

Abstract

Background DNA plasmids promise a pragmatic alternative to viral vectors for prime-boost HIV-1 vaccines. We evaluated DNA plasmid versus canarypox virus (ALVAC) primes in 2 randomized, double-blind, placebo-controlled trials in southern Africa with harmonized trial designs. HIV Vaccine Trials Network (HVTN) 111 tested DNA plasmid prime by needle or needleless injection device (Biojector) and DNA plasmid plus gp120 protein plus MF59 adjuvant boost. HVTN 100 tested ALVAC prime and ALVAC plus gp120 protein plus MF59 adjuvant boost (same protein/adjuvant as HVTN 111) by needle. Methods and findings The primary endpoints for this analysis were binding antibody (bAb) responses to HIV antigens (gp120 from strains ZM96, 1086, and TV1; variable 1 and 2 [V1V2] regions of gp120 from strains TV1, 1086, and B.CaseA, as 1086 V1V2 and B.CaseA were correlates of risk in the RV144 efficacy trial), neutralizing antibody (nAb) responses to pseudoviruses TV1c8.2 and MW925.26, and cellular responses to vaccine-matched antigens (envelope [Env] from strains ZM96, 1086, and TV1; and Gag from strains LAI and ZM96) at month 6.5, two weeks after the fourth vaccination. Per-protocol cohorts included vaccine recipients from HVTN 100 (n = 186, 60% male, median age 23 years) enrolled between February 9, 2015, and May 26, 2015 and from HVTN 111 (n = 56, 48% male, median age 24 years) enrolled between June 21, 2016, and July 13, 2017. IgG bAb response rates were 100% to 3 Env gp120 antigens in both trials. Response rates to V1V2 were lower and similar in both trials except to vaccine-matched 1086 V1V2, with rates significantly higher for the DNA-primed regimen than the ALVAC-primed regimen: 96.6% versus 72.7% (difference = 23.9%, 95% CI 15.6%–32.2%, p < 0.001). Among positive responders, bAb net mean fluorescence intensity (MFI) was significantly higher with the DNA-primed regimen than ALVAC-primed for 1086 V1V2 (geometric mean [GM] 2,833.3 versus 1,200.9; ratio = 2.36, 95% CI 1.42–3.92, p < 0.001) and B.CaseA V1V2 (GM 2314.0 versus 744.6, ratio = 3.11, 95% CI 1.51–6.38, p = 0.002). nAb response rates were >98% in both trials, with significantly higher 50% inhibitory dilution (ID50) among DNA-primed positive responders (n = 53) versus ALVAC-primed (n = 182) to tier 1A MW965.26 (GM 577.7 versus 265.7, ratio = 2.17, 95% CI 1.67–2.83, p < 0.001) and to TV1c8.2 (GM 187.3 versus 100.4, ratio = 1.87, 95% CI 1.48–2.35, p < 0.001). CD4+ T-cell response rates were significantly higher with DNA plasmid prime via Biojector than ALVAC prime (91.4% versus 52.8%, difference = 38.6%, 95% CI 20.5%–56.6%, p < 0.001 for ZM96.C; 88.0% versus 43.1%, difference = 44.9%, 95% CI 26.7%–63.1%, p < 0.001 for 1086.C; 55.5% versus 2.2%, difference = 53.3%, 95% CI 23.9%–82.7%, p < 0.001 for Gag LAI/ZM96). The study’s main limitations include the nonrandomized comparison of vaccines from 2 different trials, the lack of data on immune responses to other non–vaccine-matched antigens, and the uncertain clinical significance of the observed immunological effects. Conclusions In this study, we found that further investigation of DNA/protein regimens is warranted given enhanced immunogenicity to the V1V2 correlates of decreased HIV-1 acquisition risk identified in RV144, the only HIV vaccine trial to date to show any efficacy., Zoe Moodie and co-workers study immunological responses with DNA priming in trials of a candidate HIV vaccine., Author summary Why was this study done? HIV remains a major global health problem, especially in sub-Saharan Africa. Developing an efficacious HIV vaccine for subtype C infections, which predominate in southern Africa, is a high priority. Comparing immune responses after DNA plasmid versus viral vector priming in 2 similar subtype C HIV vaccine regimens could help inform the choice of priming strategy to use moving forward. DNA plasmid vaccines are cost-effective, easy to manufacture, and tolerable. What did the researchers do and find? We compared antibody and cellular immune responses to two phase I/II HIV-1 vaccines that differed in their priming mechanism (canarypox virus [ALVAC] vector versus DNA) but were matched in their protein boost and adjuvant. Specifically, we measured T-cell and binding and neutralizing antibody (nAb) responses to the vaccine-matched antigens from the HIV Vaccine Trials Network (HVTN) 100 and HVTN 111 trials. The vaccine regimens with DNA plasmid priming in general stimulated higher binding antibody (bAb) response magnitudes to the variable 1 and 2 (V1V2) correlates of decreased risk in RV144 and higher neutralizing responses to tier 1 viruses than the vaccine regimen with ALVAC priming. Both regimens stimulated high binding and neutralizing response rates, while DNA plasmid priming with MF59 adjuvanted protein boost induced significantly higher CD4+ T-cell response rates than ALVAC priming with MF59 adjuvanted protein boost. What do these findings mean? Our results suggest that DNA plasmid is a superior priming method for stimulating vaccine-matched humoral and cellular responses for HIV vaccine trials using this prime/boost approach. Additional investigations are warranted to optimize DNA plasmid delivery methods, such as electroporation for priming of DNA–protein combinations.

Published

2019

21. 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

22. AAV-Mediated Expression of Broadly Neutralizing and Vaccine-like Antibodies Targeting the HIV-1 Envelope V2 Region

Author

Rutendo E. Mapengo, Abdullah Ely, Bronwen E. Lambson, Tristan A. Scott, Lorraine Z. Mutsvunguma, Stuart A. Ali, Alejandro B. Balazs, Nigel A. Makoah, Lynn Morris, Salim S. Abdool Karim, Fiona T. van den Berg, Nonhlanhla N. Mkhize, Prudence Kgagudi, Marc S. Weinberg, Patrick Arbuthnot, and Carol Crowther

Subjects

0301 basic medicine, HIV vaccine, Hiv 1 envelope, Human Immunoglobulin G, Virus, Article, V2 apex, 03 medical and health sciences, 0302 clinical medicine, Genetics, gene transfer, Molecular Biology, biology, broadly neutralizing antibodies, Hiv vaccine trial, AAV, Virology, Vaccination, vectored immunoprophylaxis, 030104 developmental biology, Immunization, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Antibody

Abstract

HIV-1 infection continues to be a global health challenge and a vaccine is urgently needed. Broadly neutralizing antibodies (bNAbs) are considered essential as they inhibit multiple HIV-1 strains, but they are difficult to elicit by conventional immunization. In contrast, non-neutralizing antibodies that correlated with reduced risk of infection in the RV144 HIV vaccine trial are relatively easy to induce, but responses are not durable. To overcome these obstacles, adeno-associated virus (AAV) vectors were used to provide long-term expression of antibodies targeting the V2 region of the HIV-1 envelope protein, including the potent CAP256-VRC26.25 bNAb, as well as non-neutralizing CAP228 antibodies that resemble those elicited by vaccination. AAVs mediated effective antibody expression in cell culture and immunocompetent mice. Mean concentrations of human immunoglobulin G (IgG) in mouse sera increased rapidly following a single AAV injection, reaching 8–60 μg/mL for CAP256 antibodies and 44–220 μg/mL for CAP228 antibodies over 24 weeks, but antibody concentrations varied for individual mice. Secreted antibodies collected from serum retained the expected binding and neutralizing activity. The vectors generated here are, therefore, suitable for the delivery of V2-targeting HIV antibodies, and they could be used in a vectored immunoprophylaxis (VIP) approach to sustain the level of antibody expression required to prevent HIV infection.

Published

2018

23. Structure of an N276-Dependent HIV-1 Neutralizing Antibody Targeting a Rare V5 Glycan Hole Adjacent to the CD4 Binding Site

Author

Peter D. Kwong, Jason Gorman, Penny L. Moore, Salim S. Abdool Karim, Stephen D. Schmidt, Nonhlanhla N. Mkhize, Talita. York, Aliaksandr Druz, Phillip. Labuschagne, Mark K. Louder, Colin Anthony, John R. Mascola, Carolyn Williamson, Lynn Morris, Constantinos Kurt Wibmer, and Robert T. Bailer

Subjects

0301 basic medicine, Glycan, medicine.drug_class, Immunology, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Crystallography, X-Ray, Monoclonal antibody, Microbiology, Epitope, Virus, Cell Line, Epitopes, 03 medical and health sciences, Antigen, Polysaccharides, Virology, medicine, Humans, Binding site, Antibodies, Blocking, Neutralizing antibody, AIDS Vaccines, B-Lymphocytes, 030102 biochemistry & molecular biology, biology, Antibodies, Monoclonal, Antibodies, Neutralizing, 3. Good health, HEK293 Cells, 030104 developmental biology, Insect Science, CD4 Antigens, HIV-1, biology.protein, Pathogenesis and Immunity, Binding Sites, Antibody, Antibody

Abstract

All HIV-1-infected individuals develop strain-specific neutralizing antibodies to their infecting virus, which in some cases mature into broadly neutralizing antibodies. Defining the epitopes of strain-specific antibodies that overlap conserved sites of vulnerability might provide mechanistic insights into how broadly neutralizing antibodies arise. We previously described an HIV-1 clade C-infected donor, CAP257, who developed broadly neutralizing plasma antibodies targeting an N276 glycan-dependent epitope in the CD4 binding site. The initial CD4 binding site response potently neutralized the heterologous tier 2 clade B viral strain RHPA, which was used to design resurfaced gp120 antigens for single-B-cell sorting. Here we report the isolation and structural characterization of CAP257-RH1, an N276 glycan-dependent CD4 binding site antibody representative of the early CD4 binding site plasma response in donor CAP257. The cocrystal structure of CAP257-RH1 bound to RHPA gp120 revealed critical interactions with the N276 glycan, loop D, and V5, but not with aspartic acid 368, similarly to HJ16 and 179NC75. The CAP257-RH1 monoclonal antibody was derived from the immunoglobulin-variable IGHV3-33 and IGLV3-10 genes and neutralized RHPA but not the transmitted/founder virus from donor CAP257. Its narrow neutralization breadth was attributed to a binding angle that was incompatible with glycosylated V5 loops present in almost all HIV-1 strains, including the CAP257 transmitted/founder virus. Deep sequencing of autologous CAP257 viruses, however, revealed minority variants early in infection that lacked V5 glycans. These glycan-free V5 loops are unusual holes in the glycan shield that may have been necessary for initiating this N276 glycan-dependent CD4 binding site B-cell lineage. IMPORTANCE The conserved CD4 binding site on gp120 is a major target for HIV-1 vaccine design, but key events in the elicitation and maturation of different antibody lineages to this site remain elusive. Studies have shown that strain-specific antibodies can evolve into broadly neutralizing antibodies or in some cases act as helper lineages. Therefore, characterizing the epitopes of strain-specific antibodies may help to inform the design of HIV-1 immunogens to elicit broadly neutralizing antibodies. In this study, we isolate a narrowly neutralizing N276 glycan-dependent antibody and use X-ray crystallography and viral deep sequencing to describe how gp120 lacking glycans in V5 might have elicited these early glycan-dependent CD4 binding site antibodies. These data highlight how glycan holes can play a role in the elicitation of B-cell lineages targeting the CD4 binding site.

Published

2016

24. Broadly neutralizing antibody specificities detected in the genital tract of HIV-1 infected women

Author

Quarraisha Abdool Karim, Derseree Archary, Lynn Morris, Salim S. Abdool Karim, Penelope L. Moore, Jo-Ann S. Passmore, Nicole L. Yates, Georgia D. Tomaras, Nonhlanhla N. Mkhize, Nigel Garrett, Raveshni Durgiah, and Vicki C Ashley

Subjects

0301 basic medicine, Immunoglobulin A, Immunology, Enzyme-Linked Immunosorbent Assay, HIV Infections, HIV Antibodies, Gp41, Article, Epitope, Immunoglobulin G, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Antigen, Neutralization Tests, Humans, Immunology and Allergy, 030212 general & internal medicine, Neutralizing antibody, biology, env Gene Products, Human Immunodeficiency Virus, virus diseases, Genitalia, Female, Antibodies, Neutralizing, Virology, 030104 developmental biology, Infectious Diseases, Epitope mapping, HIV-1, biology.protein, Vaginal Douching, Female, Antibody, Epitope Mapping

Abstract

Background Broadly neutralizing antibodies (bNAbs) targeting conserved epitopes on the HIV envelope glycoprotein have been identified in blood from HIV-1 infected women. We investigated whether antibodies in the genital tract from these women share similar epitope specificities and functional profiles as those in blood. Methods Immunoglobulin (Ig)G and IgA antibodies were isolated from cervicovaginal lavages or Softcups from 13 HIV-infected women in the CAPRISA cohort using Protein G and Peptide M, respectively. Binding antibodies to envelope antigens were quantified by ELISA and binding antibody multiplex assay. Neutralizing antibody titers and epitope targets were measured using the TZM-bl assay with Env-pseudotyped wild-type and mutated viruses. Results HIV-specific IgG, but not IgA, was detected in genital secretions and the ratio of total IgG to HIV-specific IgG was similar to plasma. HIV-specific IgG reacted with multiple envelope antigens, including V1V2, gp120, gp140 and gp41. Two women had high plasma titers of HIV-specific IgG3 which was also detected in their genital tract samples. IgG from the genital tract had neutralizing activity against both Tier 1 and Tier 2 primary HIV-isolates. Antibodies targeting well known glycan epitopes and the membrane proximal region of gp41 were detected in genital secretions, and matched specificities in plasma. Conclusions Women with plasma bNAbs have overlapping specificities in their genital secretions, indicating that these predominantly IgG isotype antibodies may transudate from blood to the genital tract. These data provide evidence that induction of systemic HIV-specific bNAbs can lead to antiviral immunity at the portal of entry.

Published

2016

25. IgG3 enhances neutralization potency and Fc effector function of an HIV V2-specific broadly neutralizing antibody

Author

Mary Carrington, Margaret E. Ackerman, Salim S. Abdool Karim, Andrew R. Crowley, Nonhlanhla N. Mkhize, Nigel Garrett, Simone I. Richardson, Bronwen E. Lambson, Arman Bashirova, Penny L. Moore, Cathrine Scheepers, and Lynn Morris

Subjects

RNA viruses, Viral Diseases, Physiology, HIV Infections, Receptors, Fc, HIV Antibodies, Pathology and Laboratory Medicine, Biochemistry, Immune Receptors, Neutralization, Immunodeficiency Viruses, Immune Physiology, Medicine and Health Sciences, Enzyme-Linked Immunoassays, Biology (General), HIV vaccine, AIDS Vaccines, 0303 health sciences, Immune System Proteins, biology, 030302 biochemistry & molecular biology, Antigenic Variation, Isotype, AIDS, Immunoglobulin Isotypes, Infectious Diseases, Medical Microbiology, Cell Processes, Viral Pathogens, Viruses, Female, Pathogens, Antibody, Research Article, Signal Transduction, Adult, Trogocytosis, QH301-705.5, Immunology, Context (language use), Research and Analysis Methods, Microbiology, Antibodies, 03 medical and health sciences, Antibody Isotype, Phagocytosis, Virology, Retroviruses, Fc Receptors, Genetics, Antigenic variation, Humans, Antigens, Immunoassays, Microbial Pathogens, Molecular Biology, 030304 developmental biology, Lentivirus, Organisms, Biology and Life Sciences, Proteins, HIV, Cell Biology, RC581-607, Immunoglobulin G, Immunologic Techniques, biology.protein, Parasitology, Immunologic diseases. Allergy, Broadly Neutralizing Antibodies

Abstract

Broadly neutralizing antibodies (bNAbs) protect against HIV infection in non-human primates and their efficacy may be enhanced through interaction with Fc receptors on immune cells. Antibody isotype is a modulator of this binding with the IgG3 subclass mediating potent Fc effector function and is associated with HIV vaccine efficacy and HIV control. BNAb functions are typically assessed independently of the constant region with which they are naturally expressed. To examine the role of natural isotype in the context of a bNAb lineage we studied CAP256, an HIV-infected individual that mounted a potent V2-specific bNAb response. CAP256 expressed persistently high levels of plasma IgG3 which we found mediated both broad neutralizing activity and potent Fc function. Sequencing of germline DNA and the constant regions of V2-directed bNAbs from this donor revealed the expression of a novel IGHG3 allele as well as IGHG3*17, an allele that produces IgG3 antibodies with increased plasma half-life. Both allelic variants were used to generate CAP256-VRC26.25 and CAP256-VRC26.29 IgG3 bNAbs and these were compared to IgG1 versions. IgG3 variants were shown to have significantly higher phagocytosis and trogocytosis compared to IgG1 versions, which corresponded to increased affinity for FcγRIIa. Neutralization potency was also significantly higher for IgG3 bNAbs, particularly against viruses lacking the N160 glycan. By exchanging hinge regions between subclass variants, we showed that hinge length modulated both neutralization potency and Fc function. This study showed that co-operation between the variable and natural IgG3 constant regions enhanced the polyfunctionality of antibodies, indicating the value of leveraging genetic variation which could be exploited for passive immunity., Author summary In the only partially effective HIV vaccine trial to date, reduced risk of infection correlated with IgG3 antibodies that bound to the V2 region of the HIV envelope. IgG3 antibodies potently mediate the broadest range of Fc cytotoxic functions such as complement deposition, cellular lysis, engulfment and membrane nibbling. The relevance of different IgG3 alleles in antibody function is not typically examined, nor are antibodies usually assessed in the context of their natural isotype. Here we show that IgG3 V2-specific broadly neutralizing antibodies from donor CAP256 mediated both enhanced cytotoxic functions and neutralization potency compared to an IgG1 variant. We demonstrate that the long hinge region of IgG3 facilitated this increased functionality. These data suggest that isotype may be tuned to enhance both neutralization and cytotoxic activity of broadly neutralizing antibodies that can be used to improve the efficacy of passive immunization strategies for HIV prevention.

Published

2019

26. HIV-specific Fc effector function early in infection predicts the development of broadly neutralizing antibodies

Author

Margaret E. Ackerman, Penny L. Moore, Lynn Morris, Amy W. Chung, Harini Natarajan, Galit Alter, Nonhlanhla N. Mkhize, Nigel Garrett, Salim S. Abdool Karim, Simone I. Richardson, and Batsirai Mabvakure

Subjects

0301 basic medicine, RNA viruses, B Cells, Physiology, HIV Infections, HIV Antibodies, Pathology and Laboratory Medicine, Biochemistry, Immune Receptors, Immunoglobulin G, White Blood Cells, Immunodeficiency Viruses, Animal Cells, Immune Physiology, Medicine and Health Sciences, lcsh:QH301-705.5, Antibody-dependent cell-mediated cytotoxicity, Vaccines, Immune System Proteins, biology, Immunoglobulin Fc Fragments, Viral Load, 3. Good health, HIV Antigens, Medical Microbiology, Cell Processes, Viral Pathogens, Viruses, Infectious diseases, Antibody, Cellular Types, Pathogens, Research Article, Signal Transduction, lcsh:Immunologic diseases. Allergy, Adult, Trogocytosis, Infectious Disease Control, Immune Cells, Immunology, Viral diseases, Microbiology, Antibodies, 03 medical and health sciences, Phagocytosis, Virology, Retroviruses, Genetics, Fc Receptors, Humans, Antibody-Producing Cells, Molecular Biology, Microbial Pathogens, Blood Cells, Lentivirus, Organisms, Antibody-Dependent Cell Cytotoxicity, Germinal center, Biology and Life Sciences, Proteins, HIV, Cell Biology, Antibodies, Neutralizing, 030104 developmental biology, lcsh:Biology (General), Immunoglobulin class switching, Case-Control Studies, biology.protein, HIV-1, Parasitology, lcsh:RC581-607, Viral Transmission and Infection

Abstract

While the induction of broadly neutralizing antibodies (bNAbs) is a major goal of HIV vaccination strategies, there is mounting evidence to suggest that antibodies with Fc effector function also contribute to protection against HIV infection. Here we investigated Fc effector functionality of HIV-specific IgG plasma antibodies over 3 years of infection in 23 individuals, 13 of whom developed bNAbs. Antibody-dependent cellular phagocytosis (ADCP), complement deposition (ADCD), cellular cytotoxicity (ADCC) and cellular trogocytosis (ADCT) were detected in almost all individuals with levels of activity increasing over time. At 6 months post-infection, individuals with bNAbs had significantly higher levels of ADCD and ADCT that correlated with antibody binding to C1q and FcγRIIa respectively. In addition, antibodies from individuals with bNAbs showed more IgG subclass diversity to multiple HIV antigens which also correlated with Fc polyfunctionality. Germinal center activity represented by CXCL13 levels and expression of activation-induced cytidine deaminase (AID) was found to be associated with neutralization breadth, Fc polyfunctionality and IgG subclass diversity. Overall, multivariate analysis by random forest classification was able to group bNAb individuals with 85% sensitivity and 80% specificity based on the properties of their antibody Fc early in HIV infection. Thus, the Fc effector function profile predicted the development of neutralization breadth in this cohort, suggesting that intrinsic immune factors within the germinal center provide a mechanistic link between the Fc and Fab of HIV-specific antibodies., Author summary Some HIV-infected individuals develop antibodies that are capable of neutralizing the majority of HIV strains, a highly desirable function mediated by the antibody Fab portion. While antibodies elicited by current vaccines have failed to recreate this activity, the partial protection seen in the RV144 vaccine trial has been attributed to antibody Fc-mediated effector functions such as cell killing. In this study, we found that HIV-infected individuals who show a diversified and potent Fc response early in infection were more likely to develop broadly neutralizing antibodies later on. Examination of B cell functions associated with good germinal center activity, provided evidence for a common mechanistic link between the regulation of the Fc and Fab mediated activities in these individuals. Our finding of an Fc effector function profile that arises early and predicts neutralization breadth could be used in the evaluation of vaccine candidates designed to generate neutralizing antibodies. Common immune determinants associated with both Fab and Fc function could furthermore be exploited for vaccine design to harness the full potential of HIV-specific antibodies.

Published

2018

27. Pathology-Based Research in Africa

Author

Neil A. Martinson, Maria P. Lemos, Suzanne M. McGoldrick, Andrea Stritmatter, Julie Randolph-Habecker, Manoj Menon, Terrie E. Taylor, Steve Kussick, Nonhlanhla N. Mkhize, and Malcolm E. Molyneux

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Biomedical Research, Clinical Biochemistry, Human immunodeficiency virus (HIV), medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Acquired immunodeficiency syndrome (AIDS), parasitic diseases, medicine, Humans, Mucosal immunity, Developing Countries, Pathology, Clinical, business.industry, Biochemistry (medical), Clinical course, Diagnostic test, Clinical Laboratory Services, medicine.disease, 030104 developmental biology, Infectious disease (medical specialty), 030220 oncology & carcinogenesis, Africa, business, Malaria

Abstract

The process of conducting pathology research in Africa can be challenging. But the rewards in terms of knowledge gained, quality of collaborations, and impact on communities affected by infectious disease and cancer are great. This report reviews 3 different research efforts: fatal malaria in Malawi, mucosal immunity to HIV in South Africa, and cancer research in Uganda. What unifies them is the use of pathology-based approaches to answer vital questions, such as physiology, pathogenesis, predictors of clinical course, and diagnostic testing schemes. [Abstract copyright: Copyright © 2017 Elsevier Inc. All rights reserved.]

Published

2018

28. High rates of bacterial vaginosis and Chlamydia in a low-income, high-population-density community in Cape Town

Author

Heather B. Jaspan, Shaun L. Barnabas, Gerrit Botha, Smritee Dabee, Nicola Mulder, Jo-Ann S. Passmore, Linda-Gail Bekker, Nonhlanhla N. Mkhize, Shameem Z. Jaumdally, Glenda Gray, Enock Havyarimana, and Katie Lennard

Subjects

medicine.medical_specialty, Chlamydia, Neonatal sepsis, Obstetrics, business.industry, medicine.disease, medicine.disease_cause, female genital diseases and pregnancy complications, Group B, Streptococcus agalactiae, lcsh:Technology (General), medicine, lcsh:T1-995, lcsh:Q, Nugent score, Bacterial vaginosis, lcsh:Science, business, Prevotella amnii, Reproductive health

Abstract

Young South African women, from resource-poor communities, face several sexual and reproductive health challenges. Here we describe the vaginal microbiota and sexually transmitted infection (STI) prevalence of 102; 16–22-year-old, HIV-negative South African women from a low-income, high-population-density community in Cape Town (CPT). Vaginal microbiota were profiled using 16S rRNA amplicon sequencing; bacterial vaginosis (BV) status was established using Nugent scoring and STIs were determined by multiplex polymerase chain reaction. STIs were common, with 55% of women having at least one STI; 41% were infected with high-risk human papilloma virus (HPV) and a further 28% with low-risk HPV; 44% were infected with Chlamydia, 16% of whom had at least one additional STI. Similarly, BV rates were very high, with 55% of women classified as BV-positive (Nugent score ≥7), 7% as BV-intermediate (Nugent score 3–6) and 38% as BV-negative (Nugent 0–2). Group B Streptococcus (Streptococcus agalactiae), the leading cause of neonatal sepsis, was present in 25% of BV-positive women and 28% of BV-negative women, and was significantly more abundant among BV-negative women. Both Chlamydia infection and BV may adversely affect reproductive health and place these women at additional risk for HIV acquisition. The high abundance of Prevotella amnii, in particular, may increase HIV risk, given its inflammatory capacity. Laboratory-based testing for STIs (Chlamydia and Gonorrhoeae in particular) appear to be warranted in this community, together with further monitoring or treatment of BV.Research correlation: This article is the original version, of which an Afrikaans translation was made available to provide access to a larger readership, available here: https://doi.org/10.4102/satnt.v36i1.1495

Published

2017

29. Hoë voorkomskoers van bakteriële vaginose en Chlamydia in ’n lae-inkomste, hoë-bevolkingsdigtheid gemeenskap in Kaapstad

Author

Smritee Dabee, Nicola Mulder, Gerrit Botha, Nonhlanhla N. Mkhize, Linda-Gail Bekker, Katie Lennard, Enock Havyarimana, Jo-Ann S. Passmore, Shaun L. Barnabas, Glenda Gray, Heather B. Jaspan, and Shameem Z. Jaumdally

Subjects

Molecular cell biology, media_common.quotation_subject, lcsh:Technology (General), lcsh:T1-995, lcsh:Q, Art, Theology, lcsh:Science, media_common

Abstract

OpsommingJong Suid-Afrikaanse vroue uit hulpbron-arm gemeenskappe staar verskeie uitdagings in die gesig in terme van hulle seksuele en reproduktiewe gesondheid. Hier beskryf ons die voorkoms van vaginale mikrobiota en seksueel oordraagbare infeksies (SOI’s) onder 102; 16–22-jarige MIV-negatiewe Suid-Afrikaanse vroue uit ’n lae-inkomste, hoë-bevolkingsdigtheid gemeenskap in Kaapstad. Vaginale mikrobiota is met behulp van 16S rRNA amplikon volgorde-bepaling geprofileer; bakteriese vaginose (BV) status is met behulp van ’n Nugent-telling vasgestel; en SOI’s is deur middel van ’n multipleks polimerase kettingreaksie bepaal. SOI’s was algemeen, met 55% van die vroue wat ten minste een SOI gehad het; 41% wat met hoë-risiko menslike papillomavirus (MPV) besmet was, en ’n verdere 28% wat met laerisiko-MPV besmet was; 44% van die vroue was met Chlamydia besmet waarvan 16% een of meer addisionele SOI gehad het. BV persentasies was ook baie hoog met 55% van die vroue wat as BV-positief (Nugent-telling ≥7) geklassifiseer is, 7% as BV-intermediêr (Nugent-telling 3–6), en 38% as BV-negatief (Nugent-telling 0–2). Streptococcus (Streptococcus agalactiae), die grootste oorsaak van neonatale sepsis, was teenwoordig in 25% van die BV-positiewe vroue en 28% van die BV-negatiewe vroue, en was dus meer onder BV-negatiewe vroue. Chlamydia-infeksie sowel as BV kan reproduktiewe gesondheid nadelig beïnvloed en verhoog hierdie vroue se risiko vir die verkryging van MIV. Die voorkoms van veral Prevotella amnii kan die MIV-risiko verhoog as gevolg van sy inflammatoriese kapasiteit. Laboratorium-gebaseerde toetsing vir SOI’s (veral Chlamydia en Gonorrhoeae) blyk in hierdie gemeenskap geregverdig te wees, tesame met verdere monitering en/of behandeling van BV.Navorsing korrelasie: Hierdie artikel is die vertaalde weergawe en is beskikbaar gestel om ‘n breër lesersgroep te bereik. Die oorspronklike Engelse artikel is beskikbaar hier: https://doi.org/10.4102/satnt.v36i1.1484

Published

2017

30. Inflammatory cytokine biomarkers to identify women with asymptomatic sexually transmitted infections and bacterial vaginosis who are at high risk of HIV infection

Author

Leigh F. Johnson, Salim S. Abdool Karim, Douglas A. Lauffenburger, Sinaye Ngcapu, Jo-Ann S. Passmore, Nonhlanhla N. Mkhize, Hoyam Gamieldien, Francesca Little, Koleka Mlisana, Kelly B. Arnold, David A. Lewis, Quarraisha Abdool Karim, and Lindi Masson

Subjects

0301 basic medicine, medicine.medical_specialty, Adolescent, Interleukin-1beta, Sexually Transmitted Diseases, Cell Cycle Proteins, HIV Infections, Cervix Uteri, Dermatology, Sensitivity and Specificity, Asymptomatic, Article, Young Adult, 03 medical and health sciences, Acquired immunodeficiency syndrome (AIDS), Predictive Value of Tests, Internal medicine, Humans, Medicine, Sex organ, Young adult, Therapeutic Irrigation, business.industry, Vaginosis, Bacterial, Middle Aged, medicine.disease, Chemokine CXCL10, Cross-Sectional Studies, Logistic Models, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, ROC Curve, Predictive value of tests, Vagina, Immunology, Cytokines, Biomarker (medicine), Female, medicine.symptom, Bacterial vaginosis, business, Biomarkers

Abstract

BACKGROUND: Untreated sexually transmitted infections (STIs) and bacterial vaginosis (BV) cause genital inflammation and increased risk of HIV infection. WHO-recommended syndromic STI and BV management is severely limited as large numbers of women with asymptomatic infections go untreated. The purpose of this cross-sectional study was to evaluate genital cytokine profiles as a biomarker of STIs and BV to identify women with asymptomatic, treatable infections. METHODS: Concentrations of 42 cytokines in cervicovaginal lavages (CVL) from 227 HIV-uninfected women were measured using Luminex. All women were screened for BV by microscopy and STIs using molecular assays. Multivariate analyses were used to identify cytokine profiles associated with STIs/BV. RESULTS: A multivariate profile of seven cytokines [interleukin (IL)-1α, IL-1β, tumor necrosis factor (TNF)-β, IL-4, fractalkine, macrophage-derived chemokine (MDC), and interferon (IFN)-γ] most accurately predicted the presence of a treatable genital condition, with 77% classification accuracy and 75% cross-validation accuracy [sensitivity 72%; specificity 81%, positive predictive value (PPV) 86%, negative predictive value (NPV) 64%]. Concomitant increased IL-1β and decreased IP-10 concentrations predicted the presence of a treatable genital condition without a substantial reduction in predictive value (sensitivity 77%, specificity 72%, PPV 82% and NPV 65%), correctly classifying 75% of the women. This approach performed substantially better than clinical signs (sensitivity 19%, specificity 92%, PPV 79% and NPV 40%). CONCLUSION: Supplementing syndromic management with assessment of IL-1β and IP-10 as biomarkers of genital inflammation may improve STI/BV management for women, enabling more effective treatment of asymptomatic infections and potentially reducing their risk of HIV infection.

Published

2015

31. The carboxy-terminal tail or the intracellular loop 3 is required for β-arrestin-dependent internalization of a mammalian type II GnRH receptor

Author

Arieh A. Katz, Nonhlanhla N. Mkhize, Colleen A. Flanagan, and Michael T. Madziva

Subjects

Cytoplasm, endocrine system, genetic structures, Arrestins, Inositol Phosphates, media_common.quotation_subject, education, Biology, Biochemistry, Endocrinology, Chlorocebus aethiops, Arrestin, Animals, Internalization, Receptor, Protein kinase A, Molecular Biology, beta-Arrestins, Protein kinase C, media_common, G protein-coupled receptor, G protein-coupled receptor kinase, Cell biology, COS Cells, sense organs, Receptors, LHRH, hormones, hormone substitutes, and hormone antagonists, Intracellular, Signal Transduction

Abstract

The type II GnRH receptor (GnRH-R2) in contrast to mammalian type I GnRH receptor (GnRH-R1) has a cytosolic carboxy-terminal tail. We investigated the role of β-arrestin 1 in GnRH-R2-mediated signalling and mapped the regions in GnRH-R2 required for recruitment of β-arrestin, employing internalization assays. We show that GnRH-R2 activation of ERK is dependent on β-arrestin and protein kinase C. Appending the tail of GnRH-R2 to GnRH-R1 enabled GRK- and β-arrestin-dependent internalization of the chimaeric receptor. Surprisingly, carboxy-terminally truncated GnRH-R2 retained β-arrestin and GRK-dependent internalization, suggesting that β-arrestin interacts with additional elements of GnRH-R2. Mutating serine and threonine or basic residues of intracellular loop 3 did not abolish β-arrestin 1-dependent internalization but a receptor lacking these basic residues and the carboxy-terminus showed no β-arrestin 1-dependent internalization. Our results suggest that basic residues at the amino-terminal end of intracellular loop 3 or the carboxy-terminal tail are required for β-arrestin dependent internalization.

Published

2015

32. Microbial Composition Predicts Genital Tract Inflammation and Persistent Bacterial Vaginosis in South African Adolescent Females

Author

Gerrit Botha, Shameem Z. Jaumdally, Jo-Ann S. Passmore, Heather B. Jaspan, Anna K. Blakney, Enock Havyarimana, Katie Lennard, Nonhlanhla N. Mkhize, Shaun L. Barnabas, David A. Lewis, Linda-Gail Bekker, Glenda Gray, Smritee Dabee, and Nicola Mulder

Subjects

0301 basic medicine, Adolescent, 030106 microbiology, Immunology, Atopobium vaginae, HIV Infections, medicine.disease_cause, Microbiology, Reproductive Tract Infections, 03 medical and health sciences, Young Adult, RNA, Ribosomal, 16S, Lactobacillus iners, Prevotella, medicine, Gardnerella vaginalis, Humans, Microbiome, Genitalia, Inflammation, Host Response and Inflammation, biology, Lactobacillus crispatus, Microbiota, Vaginosis, Bacterial, biology.organism_classification, medicine.disease, Infectious Diseases, Parasitology, Female, Nugent score, Bacterial vaginosis

Abstract

Young African females are at an increased risk of HIV acquisition, and genital inflammation or the vaginal microbiome may contribute to this risk. We studied these factors in 168 HIV-negative South African adolescent females aged 16 to 22 years. Unsupervised clustering of 16S rRNA gene sequences revealed three clusters (subtypes), one of which was strongly associated with genital inflammation. In a multivariate model, the microbiome compositional subtype and hormonal contraception were significantly associated with genital inflammation. We identified 40 taxa significantly associated with inflammation, including those reported previously ( Prevotella , Sneathia , Aerococcus , Fusobacterium , and Gemella ) as well as several novel taxa (including increased frequencies of bacterial vaginosis-associated bacterium 1 [BVAB1], BVAB2, BVAB3, Prevotella amnii , Prevotella pallens , Parvimonas micra , Megasphaera , Gardnerella vaginalis , and Atopobium vaginae and decreased frequencies of Lactobacillus reuteri , Lactobacillus crispatus , Lactobacillus jensenii , and Lactobacillus iners ). Women with inflammation-associated microbiomes had significantly higher body mass indices and lower levels of endogenous estradiol and luteinizing hormone. Community functional profiling revealed three distinct vaginal microbiome subtypes, one of which was characterized by extreme genital inflammation and persistent bacterial vaginosis (BV); this subtype could be predicted with high specificity and sensitivity based on the Nugent score (≥9) or BVAB1 abundance. We propose that women with this BVAB1-dominated subtype may have chronic genital inflammation due to persistent BV, which may place them at a particularly high risk for HIV infection.

Published

2017

33. Advancing Understanding of HIV Infection in Women Through Mucosal Immunology Studies

Author

Nonhlanhla N. Mkhize, Jo-Ann S. Passmore, Derseree Archary, Lindi Masson, and Lenine L. Liebenberg

Subjects

medicine.medical_specialty, business.industry, Psychological intervention, Human immunodeficiency virus (HIV), virus diseases, medicine.disease_cause, Mucosal Infection, Microbicides for sexually transmitted diseases, Mucosal immunology, Microbicide, Immunology, CAPRISA 004, Medicine, business, Intensive care medicine, Hiv transmission

Abstract

Although women bear a disproportionate burden of HIV infection, little is known about HIV acquisition in the female reproductive tract. To bridge this gap, a structured and systematic set of mucosal immunology studies have been embedded in the CAPRISA 002 Acute Infection Study, the CAPRISA 004 and CAPRISA 008 Microbicide trials to understand heterosexual HIV transmission at the predominant site of HIV entry in women. This chapter reviews the major events from the past decade leading to the establishment of the CAPRISA Mucosal Laboratory and includes a synopsis of the key contributions this program has provided to advancing understanding of HIV infection in women. These have important implications for the design of more targeted HIV prevention interventions for women. Notable advances in understanding genital inflammation, the causes thereof, and its link to HIV acquisition are highlighted. These data are important in enhancing our understanding of the divergent pre-exposure prophylaxis (PrEP) trial findings in women and informing the development of future women-initiated HIV prevention technologies.

Published

2017

34. Subtype C gp140 Vaccine Boosts Immune Responses Primed by the South African AIDS Vaccine Initiative DNA-C2 and MVA-C HIV Vaccines after More than a 2-Year Gap

Author

Lawrence Corey, Mary Allen, Michael Pensiero, Xiaoying Shen, Carolyn Williamson, Kenneth H. Mayer, Susan W. Barnett, Georgia D. Tomaras, Nonhlanhla N. Mkhize, Niya Gu, Timothy J. Tucker, David C. Montefiori, Linda-Gail Bekker, Katrina Downing, Anna-Lise Williamson, Glenda E. Gray, Stephen C. De Rosa, Alicia Sato, Lynn Morris, and Marnie Elizaga

Subjects

0301 basic medicine, Male, Modified vaccinia Ankara, Enzyme-Linked Immunospot Assay, Time Factors, Clinical Biochemistry, MF59, HIV Antibodies, chemistry.chemical_compound, South Africa, Vaccines, DNA, Vaccinia, Immunology and Allergy, Medicine, HIV vaccine, Neutralizing antibody, AIDS Vaccines, Immunity, Cellular, Vaccines, biology, Immunogenicity, Vaccination, env Gene Products, Human Immunodeficiency Virus, 3. Good health, Female, Microbiology (medical), Adult, Adolescent, Immunology, Immunization, Secondary, complex mixtures, Injections, Intramuscular, 03 medical and health sciences, Young Adult, Humans, Immunization Schedule, Acquired Immunodeficiency Syndrome, business.industry, Virology, Antibodies, Neutralizing, CD4 Lymphocyte Count, Regimen, 030104 developmental biology, chemistry, biology.protein, HIV-1, business

Abstract

A phase I safety and immunogenicity study investigated South African AIDS Vaccine Initiative (SAAVI) HIV-1 subtype C (HIV-1C) DNA vaccine encoding Gag-RT-Tat-Nef and gp150, boosted with modified vaccinia Ankara (MVA) expressing matched antigens. Following the finding of partial protective efficacy in the RV144 HIV vaccine efficacy trial, a protein boost with HIV-1 subtype C V2-deleted gp140 with MF59 was added to the regimen. A total of 48 participants (12 U.S. participants and 36 Republic of South Africa [RSA] participants) were randomized to receive 3 intramuscular (i.m.) doses of SAAVI DNA-C2 of 4 mg (months 0, 1, and 2) and 2 i.m. doses of SAAVI MVA-C of 1.45 × 10 9 PFU (months 4 and 5) ( n = 40) or of a placebo ( n = 8). Approximately 2 years after vaccination, 27 participants were rerandomized to receive gp140/MF59 at 100 μg or placebo, as 2 i.m. injections, 3 months apart. The vaccine regimen was safe and well tolerated. After the DNA-MVA regimen, CD4 + T-cell and CD8 + T-cell responses occurred in 74% and 32% of the participants, respectively. The protein boost increased CD4 + T-cell responses to 87% of the subjects. All participants developed tier 1 HIV-1C neutralizing antibody responses as well as durable Env binding antibodies that recognized linear V3 and C5 peptides. The HIV-1 subtype C DNA-MVA vaccine regimen showed promising cellular immunogenicity. Boosting with gp140/MF59 enhanced levels of binding and neutralizing antibodies as well as CD4 + T-cell responses to HIV-1 envelope. (This study has been registered at ClinicalTrials.gov under registration no. NCT00574600 and NCT01423825.)

Published

2015

35. Persistence of Genital Tract T Cell Responses in HIV-Infected Women on Highly Active Antiretroviral Therapy

Author

Jo-Ann S. Passmore, Lenine J. P. Liebenberg, Pamela P. Gumbi, Yuan Ren, Nonhlanhla N. Mkhize, Peter G. Smith, and Lynette Denny

Subjects

Adult, CD4-Positive T-Lymphocytes, Cellular immunity, T-Lymphocytes, T cell, Immunology, HIV Infections, Viremia, Cervix Uteri, CD8-Positive T-Lymphocytes, Biology, Microbiology, South Africa, Young Adult, Immune system, Antiretroviral Therapy, Highly Active, Virology, Immunopathology, medicine, Humans, Cytotoxic T cell, Viral shedding, Cervix, virus diseases, medicine.disease, CD4 Lymphocyte Count, Virus Shedding, medicine.anatomical_structure, Insect Science, Pathogenesis and Immunity, Cytokines, Female

Abstract

Initiation of highly active antiretroviral therapy (HAART) for HIV-infected individuals is associated with control of viremia, improved CD4 counts, and declining systemic HIV-specific immune responses. While HAART effectively reduces plasma viremia, it remains unclear how effectively antiretroviral drugs reach mucosal surfaces, such as those of the genital tract. The aim of this study was to determine the effect of HAART on genital tract CD4 T cell reconstitution, HIV shedding, and HIV-specific T cell responses. Cervical cytobrush and blood specimens were obtained from 35 HIV-infected, HAART-naïve women and 27 women on HAART in order to investigate HIV Gag-specific T cell responses by intracellular gamma interferon (IFN-γ) staining. Interleukin 1β (IL-1β), IL-6, and IL-8 concentrations were measured by enzyme-linked immunosorbent assays (ELISA). We show that for HIV-infected women, HAART is associated with significantly improved CD4 T cell counts both in blood and at the cervix. While HAART effectively suppressed both blood and cervical viremia, HIV-specific CD8 T cell responses in blood were lost, while those at the cervix were preserved.

Published

2010

36. South African HIV-1 subtype C transmitted variants with a specific V2 motif show higher dependence on α4β7 for replication

Author

Simone I. Richardson, Quarraisha Abdool Karim, Jo-Ann S. Passmore, Salim S. Abdool Karim, Daniel J. Sheward, Nonhlanhla N. Mkhize, Nigel Garrett, Bronwen E. Lambson, Lise. Werner, Carolyn Williamson, Elin S. Gray, Constantinos Kurt Wibmer, Penny L. Moore, Lynn Morris, and Lindi Masson

Subjects

HIV entry, Integrins, Genotype, Gut-associated lymphoid tissue, Population, HIV Infections, HIV Envelope Protein gp120, Biology, Virus Replication, South Africa, 03 medical and health sciences, Immune system, Virology, medicine, Humans, Prospective Studies, education, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, education.field_of_study, 030306 microbiology, Research, Tripeptide-binding motif, Bacterial vaginosis, 3. Good health, α4β7, Infectious Diseases, medicine.anatomical_structure, chemistry, Viral replication, Host-Pathogen Interactions, HIV-1, biology.protein, Cytokines, Female, Antibody, Glycoprotein, Founder effect

Abstract

Background The integrin α4β7 mediates the trafficking of immune cells to the gut associated lymphoid tissue (GALT) and is an attachment factor for the HIV gp120 envelope glycoprotein. We developed a viral replication inhibition assay to more clearly evaluate the role of α4β7 in HIV infection and the contribution of viral and host factors. Results Replication of 60 HIV-1 subtype C viruses collected over time from 11 individuals in the CAPRISA cohort were partially inhibited by antibodies targeting α4β7. However, dependence on α4β7 for replication varied substantially among viral isolates from different individuals as well as over time in some individuals. Among 8 transmitted/founder (T/F) viruses, α4β7 reactivity was highest for viruses having P/SDI/V tri-peptide binding motifs. Mutation of T/F viruses that had LDI/L motifs to P/SDI/V resulted in greater α4β7 reactivity, whereas mutating P/SDI/V to LDI/L motifs was associated with reduced α4β7 binding. P/SDI/V motifs were more common among South African HIV subtype C viruses (35%) compared to subtype C viruses from other regions of Africa (

Published

2015

37. Reactivity of routine HIV antibody tests in children who initiated antiretroviral therapy in early infancy as part of the Children with HIV Early Antiretroviral Therapy (CHER) trial

Author

Robin E. Callard, Avy Violari, Helen Payne, Lynn Morris, Ravindre Panchia, Joanna Lewis, Abdel Babiker, Nigel Klein, Mark F. Cotton, Kennedy Otwombe, Diana M. Gibb, and Nonhlanhla N. Mkhize

Subjects

Male, Pediatrics, medicine.medical_specialty, Time Factors, Anti-HIV Agents, Enzyme-Linked Immunosorbent Assay, HIV Antibodies, Chromatography, Affinity, Article, law.invention, Randomized controlled trial, law, HIV Seronegativity, HIV Seropositivity, medicine, Humans, Retrospective Studies, biology, medicine.diagnostic_test, business.industry, AIDS Serodiagnosis, Infant, Retrospective cohort study, Viral Load, Antiretroviral therapy, CD4 Lymphocyte Count, Clinical trial, Infectious Diseases, Immunoassay, Immunology, HIV-2, biology.protein, HIV-1, Female, Antibody, business, Viral load

Abstract

Early antiretroviral therapy (ART) and virological suppression can affect evolving antibody responses to HIV infection. We aimed to assess frequency and predictors of seronegativity in infants starting early ART.We compared HIV antibody results between two of three treatment groups of the Children with HIV Early Antiretroviral Therapy (CHER) trial, done from July, 2005, until July, 2011, in which infants with HIV infection aged 5·7-12·0 weeks with a percentage of CD4-positive T lymphocytes of at least 25% were randomly assigned to immediate ART for 96 weeks (ART-96W) or deferred ART until clinical or immunological progression (ART-Def). We measured antibody from all available stored samples for ART-96W and ART-Def at trial week 84 using three assays: fourth-generation enzyme immunoassay HIV antigen-antibody combination, HIV-1 and HIV-2 rapid antibody test, and quantitative anti-gp120 IgG ELISA. We also assessed odds of seropositivity with respect to age of ART initiation and cumulative viral load. The CHER trial was registered with ClinicalTrials.gov, number NCT00102960.The median age of the infants from when samples were taken (184 samples from 268 infants) was 92 weeks (IQR 90·6-93·4). More specimens from the ART-96W group were seronegative than from the ART-Def group by enzyme immunoassay (ART-96W 49 [46%] of 107 vs ART-Def eight [11%] of 75; p0·0001) and rapid antibody test (54 [53%] of 101 vs eight [11%] of 74; p0·0001). Median anti-gp120 IgG concentration was lower in the ART-96W group (230 μg/μL [IQR 133-13 129]) than in the ART-Def group (6870 μg/μL [1706-53 645]; p0·0001). If ART was started between 12 and 24 weeks of age, odds of seropositivity were increased 13·7 times (95% CI 3·1-60·2; p=0·001) compared with starting it between 0 and 12 weeks. All children starting ART aged older than 24 weeks were seropositive. Cumulative viral load to week 84 correlated with anti-gp120 IgG concentrations (coefficient 0·54; p0·0001) and increased odds of seropositivity (odds ratio 1·59 [95% CI 1·1-2·3]) adjusted for ART initiation age.About half of children starting ART before 12 weeks of age were HIV seronegative by almost 2 years of age. HIV antibody tests cannot be used to reconfirm HIV diagnosis in children starting early ART. Long-term effects of seronegativity need further study. Clear guidelines are needed for retesting alongside improved diagnostic tests.Wellcome Trust, Medical Research Council, and National Institutes of Health.

Published

2015

38. Defining genital tract cytokine signatures of sexually transmitted infections and bacterial vaginosis in women at high risk of HIV infection: a cross-sectional study

Author

Lyle R. McKinnon, Quarraisha Abdool Karim, Carolyn Williamson, Lise. Werner, Lindi Masson, Salim S. Abdool Karim, Francesca Little, Katharina Ronacher, Nonhlanhla N. Mkhize, Koleka Mlisana, Gerhard Walzl, Hoyam Gamieldien, and Jo-Ann S. Passmore

Subjects

Adult, Adolescent, medicine.medical_treatment, Herpesvirus 2, Human, Sexually Transmitted Diseases, Chlamydia trachomatis, Dermatology, urologic and male genital diseases, medicine.disease_cause, Proinflammatory cytokine, Young Adult, Acquired immunodeficiency syndrome (AIDS), medicine, Trichomonas vaginalis, Humans, Chlamydia, Trichomoniasis, business.industry, Vaginosis, Bacterial, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Neisseria gonorrhoeae, Infectious Diseases, Cytokine, Blood, Cross-Sectional Studies, Immunology, Vagina, Cytokines, Female, Bacterial vaginosis, business

Abstract

Objectives Sexually transmitted infections (STI) and bacterial vaginosis (BV) cause female genital tract inflammation. This inflammation, which is often present in the absence of symptoms, is associated with increased susceptibility to HIV infection. We aimed to evaluate genital cytokine profiles and the degree of inflammation associated with common STIs and BV. Methods HIV-uninfected women (n=227) were screened for BV, Chlamydia trachomatis , Neisseria gonorrhoeae , Herpes simplex virus type 2 (HSV-2), and Trichomonas vaginalis . Concentrations of 42 cytokines in cervicovaginal lavages and 13 cytokines in plasma were measured using Luminex. Changes in cytokine profiles were evaluated using Mann–Whitney U test, logistic regression and factor analysis. p Values were adjusted for multiple comparisons using a false discovery rate step-down procedure. Results Women with chlamydia or gonorrhoea had the highest genital cytokine concentrations, with 17/42 and 14/42 cytokines upregulated compared with women with no infection, respectively. BV was associated with elevated proinflammatory cytokine concentrations, but lower chemokine and haematopoietic cytokine concentrations. HSV-2 reactivation was associated with lower levels of inflammation, while trichomoniasis did not cause significant differences in genital cytokine concentrations. Genital infections did not influence plasma cytokine concentrations. Although certain STIs, in particular chlamydia and gonorrhoea, were associated with high genital cytokine concentrations, only 19% of women with an STI/BV had clinical signs. Conclusions Chlamydia was associated with the highest genital cytokine levels, followed by gonorrhoea, HSV-2, trichomoniasis, and BV. In regions where HIV is prevalent and STIs are managed syndromically, better STI/BV screening is urgently needed, as certain infections were found to be highly inflammatory.

Published

2014

39. Sequential Immunization with gp140 Boosts Immune Responses Primed by Modified Vaccinia Ankara or DNA in HIV-Uninfected South African Participants

Author

Tandile Hermanus, Koleka Mlisana, Nonhlanhla N. Mkhize, Gavin J. Churchyard, Georgia D. Tomaras, Niya Gu, Peter B. Gilbert, Shelly Karuna, Lawrence Corey, Stephen C. De Rosa, Susan W. Barnett, Mary Allen, James G. Kublin, David C. Montefiori, Linda-Gail Bekker, Carolyn Williamson, Anna-Lise Williamson, Chenchen Yu, Glenda Gray, Michael Pensiero, Lynn Morris, Division of Virology, and Faculty of Health Sciences

Subjects

CD4-Positive T-Lymphocytes, Male, 0301 basic medicine, Modified vaccinia Ankara, Time Factors, Physiology, medicine.medical_treatment, MF59, lcsh:Medicine, Antibody Response, CD8-Positive T-Lymphocytes, Biochemistry, White Blood Cells, South Africa, 0302 clinical medicine, Animal Cells, Pregnancy, Immune Physiology, HIV Seropositivity, Medicine and Health Sciences, Vaccines, DNA, Vaccinia, Public and Occupational Health, 030212 general & internal medicine, lcsh:Science, Immune Response, Vaccines, Immune System Proteins, Multidisciplinary, biology, T Cells, Immunogenicity, env Gene Products, Human Immunodeficiency Virus, Vaccination and Immunization, 3. Good health, Vaccination, Female, Cellular Types, Safety, Antibody, Adjuvant, Research Article, Adult, Adolescent, Immune Cells, Immunology, Immunization, Secondary, complex mixtures, Antibodies, Young Adult, 03 medical and health sciences, Immune system, Antigen, DNA-binding proteins, medicine, Humans, Antigens, Blood Cells, lcsh:R, Biology and Life Sciences, Proteins, Cell Biology, Antibodies, Neutralizing, Virology, 030104 developmental biology, HIV-1, biology.protein, lcsh:Q, Preventive Medicine

Abstract

Background The safety and immunogenicity of SAAVI DNA-C2 (4 mg IM), SAAVI MVA-C (2.9 x 109 pfu IM) and Novartis V2-deleted subtype C gp140 (100 mcg) with MF59 adjuvant in various vaccination regimens was evaluated in HIV-uninfected adults in South Africa. Methods Participants at three South African sites were randomized (1:1:1:1) to one of four vaccine regimens: MVA prime, sequential gp140 protein boost (M/M/P/P); concurrent MVA/gp140 (MP/MP); DNA prime, sequential MVA boost (D/D/M/M); DNA prime, concurrent MVA/gp140 boost (D/D/MP/MP) or placebo. Peak HIV specific humoral and cellular responses were measured. Results 184 participants were enrolled: 52% were female, all were Black/African, median age was 23 years (range, 18–42 years) and 79% completed all vaccinations. 159 participants reported at least one adverse event, 92.5% were mild or moderate. Five, unrelated, serious adverse events were reported. The M/M/P/P and D/D/MP/MP regimens induced the strongest peak neutralizing and binding antibody responses and the greatest CD4+ T-cell responses to Env. All peak neutralizing and binding antibody responses decayed with time. The MVA, but not DNA, prime contributed to the humoral and cellular immune responses. The D/D/M/M regimen was poorly immunogenic overall but did induce modest CD4+ T-cell responses to Gag and Pol. CD8+ T-cell responses to any antigen were low for all regimens. Conclusions The SAAVI DNA-C2, SAAVI MVA-C and Novartis gp140 with MF59 adjuvant in various combinations were safe and induced neutralizing and binding antibodies and cellular immune responses. Sequential immunization with gp140 boosted immune responses primed by MVA or DNA. The best overall immune responses were seen with the M/M/P/P regimen. Trial Registration ClinicalTrials.gov NCT01418235

Published

2016

40. P06.13 Inflammatory cytokine biomarkers identify women with asymptomatic genital infections that increase the risk of hiv infection

Author

Doug A. Lauffenburger, L Van Damme, S. S. Abdool Karim, Lindi Masson, Jennifer Deese, Q. Abdool Karim, Francesca Little, Sinaye Ngcapu, Koleka Mlisana, Tania Crucitti, Kelly B. Arnold, JS Passmore, Nonhlanhla N. Mkhize, Hoyam Gamieldien, David A. Lewis, and Saïd Abdellati

Subjects

medicine.medical_specialty, biology, business.industry, Dermatology, medicine.disease, medicine.disease_cause, biology.organism_classification, Asymptomatic, Poliomyelitis, Infectious Diseases, Acquired immunodeficiency syndrome (AIDS), Internal medicine, Immunology, medicine, Trichomonas vaginalis, Bacterial vaginosis, medicine.symptom, Chlamydia trachomatis, business, Mycoplasma genitalium, Reproductive health

Abstract

Introduction Untreated sexually transmitted infections (STIs) and bacterial vaginosis (BV) cause genital inflammation and increased risk of HIV infection. WHO-recommended syndromic STI and BV management is limited as large numbers of women with asymptomatic infections go untreated. The purpose of this study was to evaluate genital cytokine profiles as a biomarker to identify women with asymptomatic, treatable infections. Methods Luminex was used to measure the concentrations of 42 cytokines in cervicovaginal lavages (CVL) from 227 HIV-uninfected women from Durban, South Africa, and nine cytokines in endocervical swabs from 264 women from Bondo, Kenya and Pretoria, South Africa. Women were screened for BV and treatable STIs ( Chlamydia trachomatis , Neisseria gonorrhoeae , Trichomonas vaginalis , Mycoplasma genitalium ) using microscopy and molecular assays. Nonparametric receiver operating characteristic curves and logistic regression were used to identify cytokine profiles associated with STIs/BV. Results In women from Durban, concomitant increased IL-1α and IL-1β and decreased IP-10 concentrations in CVLs predicted the presence of a treatable genital condition, correctly classifying 76% of women (sensitivity 72%, specificity 81%, PPV 86% and NPV 64%). In a separate validation cohort of women from Bondo and Pretoria, IL-1α, IL-1β and IP-10 concentrations in endocervical swabs correctly classified 72% of the participants according to STI/BV status. This approach performed substantially better than clinical signs in both cohorts from Durban (sensitivity 19%, specificity 92%, PPV 79% and NPV 40%) and Pretoria and Bondo (sensitivity 29%, specificity 78%, PPV 68%, NPV 39%). Conclusion Across two cohorts of women residing in different regions in sub-Saharan Africa, genital IL-1α, IL-1β and IP-10 together was the best immunological predictor of the presence of an STI or BV. Supplementing syndromic management with point-of-care assessment of biomarkers of genital inflammation may improve STI/BV management for women, enabling more effective treatment of asymptomatic infections and potentially reducing their risk of HIV infection. Disclosure of interest statement This work was supported by a Strategic Health Innovation Partnerships (SHIP) grant from the South African Medical Research Council and grants from the Poliomyelitis Research Foundation (PRF) of South Africa and European and Developing Countries Clinical Trials Partnership (EDCTP). The cohorts were supported by grants from the Comprehensive International Program of Research on AIDS (CIPRA) of the Division of AIDS (DAIDS); National Institute of Allergy and infectious Disease (NIAID); National Institutes of Health (NIH) and US Department of Health and Human Services (DHHS) [grant number U19 AI51794]. FEM-PrEP was conducted under two grants funded by the United States Agency for International Development (USAID): the Contraceptive and Reproductive Health Technologies and Research Utilisation Program (GPO-A-00–05–00022–00), and the Preventive Technologies Agreement (GHO-A-00–09–00016–00). Early support was also provided by the Bill and Melinda Gates Foundation. Gilead Sciences, Inc. donated Truvada® and placebo. LM was supported by the PRF; South African Medical Research Council (MRC); the Carnegie Corporation; the National Research Foundation (NRF) of South Africa and the UCT Clinical Infectious Diseases Research Initiative/Wellcome Trust. No pharmaceutical grants were received in the development of this study.

Published

2015

41. Comparison of the neutralization sensitivity of South African and Indian HIV-1 subtype C viruses to South African plasma antibodies

Author

Lynn Morris, Penelope L. Moore, Nonhlanhla N. Mkhize, Molati Nonyane, T Hermanus, J Battacharya, and Salim S. Abdool Karim

Subjects

lcsh:Immunologic diseases. Allergy, Veterinary medicine, biology, business.industry, Human immunodeficiency virus (HIV), Acute infection, medicine.disease_cause, Virology, Epitope, Neutralization, Infectious Diseases, Poster Presentation, medicine, biology.protein, Antibody, business, lcsh:RC581-607

Abstract

Methods Plasma from 44 chronically HIV-1 subtype C infected SA individuals in the CAPRISA 002 Acute Infection cohort were used to assess the neutralization sensitivity of 10 SA and 9 Indian Tier 2 viruses in a TZM-bl assay. Intra-subtype neutralization activity between SA and Indian viruses was determined. The envelope sequence of the Indian panel was analyzed in order to identify epitopes known to be targeted by the neutralizing antibodies in a subset of the CAPRISA plasmas.

Published

2012

42. Stability and transport of cervical cytobrushes for isolation of mononuclear cells from the female genital tract

Author

Lenine J. P. Liebenberg, Hoyam Gamieldien, Lynette Denny, Pam P. Gumbi, Nonhlanhla N. Mkhize, Shameem Z. Jaumdally, and Jo-Ann S. Passmore

Subjects

Adult, Yield, Cytobrush, Cell Survival, T cell, CD3, T-Lymphocytes, Immunology, HIV Infections, Cell Separation, Cervix Uteri, Peripheral blood mononuclear cell, Cryopreservation, Specimen Handling, Andrology, 03 medical and health sciences, Interferon-gamma, 0302 clinical medicine, Immune system, Antigen, medicine, Humans, Immunology and Allergy, Lymphocyte Count, 030304 developmental biology, 0303 health sciences, biology, Genital tract, T lymphocyte, 3. Good health, medicine.anatomical_structure, biology.protein, Female, Ex vivo, 030215 immunology, Research Paper

Abstract

Cervical cytobrushing, biopsy, or lavages have previously been used to collect mononuclear cells from the female genital tract. Compared with blood, obtaining cells from the female genital tract is more invasive and generally yields few cells for subsequent immune studies. Because of the value of including mucosal sampling in HIV vaccine trials, standardisation of methods for collection, processing, and analysis of immunity from cells derived from the female genital tract is important. The aim of this study was to assess the effect of transport conditions on the viability, recovery and antigenic responsiveness of cervical T cells. This was investigated in cervical cytobrush specimens collected from 215 chronically HIV-infected women. Cytobrushes were either processed immediately, after cryopreservation, or after 24h at 37°C, 4°C or room temperature. CD3+ T cell numbers were quantified using Guava automated cell counting. Viability was assessed using Trypan and Annexin/PI staining. Intracellular cytokine staining was used to evaluate IFN-γ responses to PMA, PHA and CEF peptides in cytobrush-derived T cells ex vivo and after delayed processing. In vitro polyclonal expansion of thawed cervical lymphocytes was conducted for 14days in the presence of anti-CD3 and IL-2. We found that CD3+ T cell recovery and viability was similar in cytobrushes processed immediately or after 24h irrespective of the conditions at which they were maintained. Fifty percent of the CD3+ T cells could be recovered after cryopreservation of cytobrushes and these could be polyclonally expanded in half of the cryopreserved samples. IFN-γ production following mitogenic stimulation was similar in ex vivo and delayed processing cytobrushes. Maintaining cytobrushes at 37°C prior to processing significantly improved the detection of CEF-specific T cell responses compared to ex vivo. We conclude that cervical cytobrush-derived T cells are robust and can preserve their viability, phenotype and function over 24h of mock transport.

43. Neutralization profiles of HIV-1 viruses from the VRC01 Antibody Mediated Prevention (AMP) trials.

Author

Nonhlanhla N Mkhize, Anna E J Yssel, Haajira Kaldine, Rebecca T van Dorsten, Amanda S Woodward Davis, Nicolas Beaume, David Matten, Bronwen Lambson, Tandile Modise, Prudence Kgagudi, Talita York, Dylan H Westfall, Elena E Giorgi, Bette Korber, Colin Anthony, Rutendo E Mapengo, Valerie Bekker, Elizabeth Domin, Amanda Eaton, Wenjie Deng, Allan DeCamp, Yunda Huang, Peter B Gilbert, Asanda Gwashu-Nyangiwe, Ruwayhida Thebus, Nonkululeko Ndabambi, Dieter Mielke, Nyaradzo Mgodi, Shelly Karuna, Srilatha Edupuganti, Michael S Seaman, Lawrence Corey, Myron S Cohen, John Hural, M Juliana McElrath, James I Mullins, David Montefiori, Penny L Moore, Carolyn Williamson, and Lynn Morris

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The VRC01 Antibody Mediated Prevention (AMP) efficacy trials conducted between 2016 and 2020 showed for the first time that passively administered broadly neutralizing antibodies (bnAbs) could prevent HIV-1 acquisition against bnAb-sensitive viruses. HIV-1 viruses isolated from AMP participants who acquired infection during the study in the sub-Saharan African (HVTN 703/HPTN 081) and the Americas/European (HVTN 704/HPTN 085) trials represent a panel of currently circulating strains of HIV-1 and offer a unique opportunity to investigate the sensitivity of the virus to broadly neutralizing antibodies (bnAbs) being considered for clinical development. Pseudoviruses were constructed using envelope sequences from 218 individuals. The majority of viruses identified were clade B and C; with clades A, D, F and G and recombinants AC and BF detected at lower frequencies. We tested eight bnAbs in clinical development (VRC01, VRC07-523LS, 3BNC117, CAP256.25, PGDM1400, PGT121, 10-1074 and 10E8v4) for neutralization against all AMP placebo viruses (n = 76). Compared to older clade C viruses (1998-2010), the HVTN703/HPTN081 clade C viruses showed increased resistance to VRC07-523LS and CAP256.25. At a concentration of 1μg/ml (IC80), predictive modeling identified the triple combination of V3/V2-glycan/CD4bs-targeting bnAbs (10-1074/PGDM1400/VRC07-523LS) as the best against clade C viruses and a combination of MPER/V3/CD4bs-targeting bnAbs (10E8v4/10-1074/VRC07-523LS) as the best against clade B viruses, due to low coverage of V2-glycan directed bnAbs against clade B viruses. Overall, the AMP placebo viruses represent a valuable resource for defining the sensitivity of contemporaneous circulating viral strains to bnAbs and highlight the need to update reference panels regularly. Our data also suggests that combining bnAbs in passive immunization trials would improve coverage of global viruses.

Published

2023

44. Antibody and cellular responses to HIV vaccine regimens with DNA plasmid as compared with ALVAC priming: An analysis of two randomized controlled trials.

Author

Zoe Moodie, Stephen R Walsh, Fatima Laher, Lucas Maganga, Michael E Herce, Sarita Naidoo, Mina C Hosseinipour, Craig Innes, Linda-Gail Bekker, Nicole Grunenberg, Philipp Mann, Chenchen Yu, Allan C deCamp, Maurine D Miner, Nicole L Yates, Jack Heptinstall, Nonhlanhla N Mkhize, One Dintwe, Nicole Frahm, Kristen W Cohen, Mary Allen, Julia Hutter, Ralf Wagner, Giuseppe Pantaleo, M Juliana McElrath, Georgia D Tomaras, Lynn Morris, David C Montefiori, Erica Andersen-Nissen, Glenda E Gray, Peter B Gilbert, James G Kublin, and NIAID HVTN 100 and HVTN 111 trial teams

Subjects

Medicine

Abstract

BackgroundDNA plasmids promise a pragmatic alternative to viral vectors for prime-boost HIV-1 vaccines. We evaluated DNA plasmid versus canarypox virus (ALVAC) primes in 2 randomized, double-blind, placebo-controlled trials in southern Africa with harmonized trial designs. HIV Vaccine Trials Network (HVTN) 111 tested DNA plasmid prime by needle or needleless injection device (Biojector) and DNA plasmid plus gp120 protein plus MF59 adjuvant boost. HVTN 100 tested ALVAC prime and ALVAC plus gp120 protein plus MF59 adjuvant boost (same protein/adjuvant as HVTN 111) by needle.Methods and findingsThe primary endpoints for this analysis were binding antibody (bAb) responses to HIV antigens (gp120 from strains ZM96, 1086, and TV1; variable 1 and 2 [V1V2] regions of gp120 from strains TV1, 1086, and B.CaseA, as 1086 V1V2 and B.CaseA were correlates of risk in the RV144 efficacy trial), neutralizing antibody (nAb) responses to pseudoviruses TV1c8.2 and MW925.26, and cellular responses to vaccine-matched antigens (envelope [Env] from strains ZM96, 1086, and TV1; and Gag from strains LAI and ZM96) at month 6.5, two weeks after the fourth vaccination. Per-protocol cohorts included vaccine recipients from HVTN 100 (n = 186, 60% male, median age 23 years) enrolled between February 9, 2015, and May 26, 2015 and from HVTN 111 (n = 56, 48% male, median age 24 years) enrolled between June 21, 2016, and July 13, 2017. IgG bAb response rates were 100% to 3 Env gp120 antigens in both trials. Response rates to V1V2 were lower and similar in both trials except to vaccine-matched 1086 V1V2, with rates significantly higher for the DNA-primed regimen than the ALVAC-primed regimen: 96.6% versus 72.7% (difference = 23.9%, 95% CI 15.6%-32.2%, p < 0.001). Among positive responders, bAb net mean fluorescence intensity (MFI) was significantly higher with the DNA-primed regimen than ALVAC-primed for 1086 V1V2 (geometric mean [GM] 2,833.3 versus 1,200.9; ratio = 2.36, 95% CI 1.42-3.92, p < 0.001) and B.CaseA V1V2 (GM 2314.0 versus 744.6, ratio = 3.11, 95% CI 1.51-6.38, p = 0.002). nAb response rates were >98% in both trials, with significantly higher 50% inhibitory dilution (ID50) among DNA-primed positive responders (n = 53) versus ALVAC-primed (n = 182) to tier 1A MW965.26 (GM 577.7 versus 265.7, ratio = 2.17, 95% CI 1.67-2.83, p < 0.001) and to TV1c8.2 (GM 187.3 versus 100.4, ratio = 1.87, 95% CI 1.48-2.35, p < 0.001). CD4+ T-cell response rates were significantly higher with DNA plasmid prime via Biojector than ALVAC prime (91.4% versus 52.8%, difference = 38.6%, 95% CI 20.5%-56.6%, p < 0.001 for ZM96.C; 88.0% versus 43.1%, difference = 44.9%, 95% CI 26.7%-63.1%, p < 0.001 for 1086.C; 55.5% versus 2.2%, difference = 53.3%, 95% CI 23.9%-82.7%, p < 0.001 for Gag LAI/ZM96). The study's main limitations include the nonrandomized comparison of vaccines from 2 different trials, the lack of data on immune responses to other non-vaccine-matched antigens, and the uncertain clinical significance of the observed immunological effects.ConclusionsIn this study, we found that further investigation of DNA/protein regimens is warranted given enhanced immunogenicity to the V1V2 correlates of decreased HIV-1 acquisition risk identified in RV144, the only HIV vaccine trial to date to show any efficacy.

Published

2020

45. 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

46. IgG3 enhances neutralization potency and Fc effector function of an HIV V2-specific broadly neutralizing antibody.

Author

Simone I Richardson, Bronwen E Lambson, Andrew R Crowley, Arman Bashirova, Cathrine Scheepers, Nigel Garrett, Salim Abdool Karim, Nonhlanhla N Mkhize, Mary Carrington, Margaret E Ackerman, Penny L Moore, and Lynn Morris

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Broadly neutralizing antibodies (bNAbs) protect against HIV infection in non-human primates and their efficacy may be enhanced through interaction with Fc receptors on immune cells. Antibody isotype is a modulator of this binding with the IgG3 subclass mediating potent Fc effector function and is associated with HIV vaccine efficacy and HIV control. BNAb functions are typically assessed independently of the constant region with which they are naturally expressed. To examine the role of natural isotype in the context of a bNAb lineage we studied CAP256, an HIV-infected individual that mounted a potent V2-specific bNAb response. CAP256 expressed persistently high levels of plasma IgG3 which we found mediated both broad neutralizing activity and potent Fc function. Sequencing of germline DNA and the constant regions of V2-directed bNAbs from this donor revealed the expression of a novel IGHG3 allele as well as IGHG3*17, an allele that produces IgG3 antibodies with increased plasma half-life. Both allelic variants were used to generate CAP256-VRC26.25 and CAP256-VRC26.29 IgG3 bNAbs and these were compared to IgG1 versions. IgG3 variants were shown to have significantly higher phagocytosis and trogocytosis compared to IgG1 versions, which corresponded to increased affinity for FcγRIIa. Neutralization potency was also significantly higher for IgG3 bNAbs, particularly against viruses lacking the N160 glycan. By exchanging hinge regions between subclass variants, we showed that hinge length modulated both neutralization potency and Fc function. This study showed that co-operation between the variable and natural IgG3 constant regions enhanced the polyfunctionality of antibodies, indicating the value of leveraging genetic variation which could be exploited for passive immunity.

Published

2019

47. HIV-specific Fc effector function early in infection predicts the development of broadly neutralizing antibodies.

Author

Simone I Richardson, Amy W Chung, Harini Natarajan, Batsirai Mabvakure, Nonhlanhla N Mkhize, Nigel Garrett, Salim Abdool Karim, Penny L Moore, Margaret E Ackerman, Galit Alter, and Lynn Morris

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

While the induction of broadly neutralizing antibodies (bNAbs) is a major goal of HIV vaccination strategies, there is mounting evidence to suggest that antibodies with Fc effector function also contribute to protection against HIV infection. Here we investigated Fc effector functionality of HIV-specific IgG plasma antibodies over 3 years of infection in 23 individuals, 13 of whom developed bNAbs. Antibody-dependent cellular phagocytosis (ADCP), complement deposition (ADCD), cellular cytotoxicity (ADCC) and cellular trogocytosis (ADCT) were detected in almost all individuals with levels of activity increasing over time. At 6 months post-infection, individuals with bNAbs had significantly higher levels of ADCD and ADCT that correlated with antibody binding to C1q and FcγRIIa respectively. In addition, antibodies from individuals with bNAbs showed more IgG subclass diversity to multiple HIV antigens which also correlated with Fc polyfunctionality. Germinal center activity represented by CXCL13 levels and expression of activation-induced cytidine deaminase (AID) was found to be associated with neutralization breadth, Fc polyfunctionality and IgG subclass diversity. Overall, multivariate analysis by random forest classification was able to group bNAb individuals with 85% sensitivity and 80% specificity based on the properties of their antibody Fc early in HIV infection. Thus, the Fc effector function profile predicted the development of neutralization breadth in this cohort, suggesting that intrinsic immune factors within the germinal center provide a mechanistic link between the Fc and Fab of HIV-specific antibodies.

Published

2018

48. Prospects for passive immunity to prevent HIV infection.

Author

Lynn Morris and Nonhlanhla N Mkhize

Subjects

Medicine

Abstract

In a Perspective, Lynn Morris and Nonhlanhla Mkhize discuss the prospects for broadly neutralizing antibodies to be used in preventing HIV infection.

Published

2017

49. Sequential Immunization with gp140 Boosts Immune Responses Primed by Modified Vaccinia Ankara or DNA in HIV-Uninfected South African Participants.

Author

Gavin Churchyard, Koleka Mlisana, Shelly Karuna, Anna-Lise Williamson, Carolyn Williamson, Lynn Morris, Georgia D Tomaras, Stephen C De Rosa, Peter B Gilbert, Niya Gu, Chenchen Yu, Nonhlanhla N Mkhize, Tandile Hermanus, Mary Allen, Michael Pensiero, Susan W Barnett, Glenda Gray, Linda-Gail Bekker, David C Montefiori, James Kublin, and Lawrence Corey

Subjects

Medicine, Science

Abstract

BACKGROUND:The safety and immunogenicity of SAAVI DNA-C2 (4 mg IM), SAAVI MVA-C (2.9 x 109 pfu IM) and Novartis V2-deleted subtype C gp140 (100 mcg) with MF59 adjuvant in various vaccination regimens was evaluated in HIV-uninfected adults in South Africa. METHODS:Participants at three South African sites were randomized (1:1:1:1) to one of four vaccine regimens: MVA prime, sequential gp140 protein boost (M/M/P/P); concurrent MVA/gp140 (MP/MP); DNA prime, sequential MVA boost (D/D/M/M); DNA prime, concurrent MVA/gp140 boost (D/D/MP/MP) or placebo. Peak HIV specific humoral and cellular responses were measured. RESULTS:184 participants were enrolled: 52% were female, all were Black/African, median age was 23 years (range, 18-42 years) and 79% completed all vaccinations. 159 participants reported at least one adverse event, 92.5% were mild or moderate. Five, unrelated, serious adverse events were reported. The M/M/P/P and D/D/MP/MP regimens induced the strongest peak neutralizing and binding antibody responses and the greatest CD4+ T-cell responses to Env. All peak neutralizing and binding antibody responses decayed with time. The MVA, but not DNA, prime contributed to the humoral and cellular immune responses. The D/D/M/M regimen was poorly immunogenic overall but did induce modest CD4+ T-cell responses to Gag and Pol. CD8+ T-cell responses to any antigen were low for all regimens. CONCLUSIONS:The SAAVI DNA-C2, SAAVI MVA-C and Novartis gp140 with MF59 adjuvant in various combinations were safe and induced neutralizing and binding antibodies and cellular immune responses. Sequential immunization with gp140 boosted immune responses primed by MVA or DNA. The best overall immune responses were seen with the M/M/P/P regimen. TRIAL REGISTRATION:ClinicalTrials.gov NCT01418235.

Published

2016

50. Safety and immunogenicity of the ChAdOx1 nCoV-19 (AZD1222) vaccine against SARS-CoV-2 in people living with and without HIV in South Africa: an interim analysis of a randomised, double-blind, placebo-controlled, phase 1B/2A trial.

Author

Madhi SA, Koen AL, Izu A, Fairlie L, Cutland CL, Baillie V, Padayachee SD, Dheda K, Barnabas SL, Bhorat QE, Briner C, Aley PK, Bhikha S, Hermanus T, Horne E, Jose A, Kgagudi P, Lambe T, Masenya M, Masilela M, Mkhize N, Moultrie A, Mukendi CK, Moyo-Gwete T, Nana AJ, Nzimande A, Patel F, Rhead S, Taoushanis C, Thombrayil A, van Eck S, Voysey M, Villafana TL, Vekemans J, Gilbert SC, Pollard AJ, Moore PL, and Kwatra G

Subjects

Adult, Antibodies, Neutralizing blood, Antibodies, Viral blood, COVID-19 epidemiology, COVID-19 Vaccines administration & dosage, COVID-19 Vaccines adverse effects, ChAdOx1 nCoV-19, Cross Reactions, Double-Blind Method, Female, Humans, Immunogenicity, Vaccine, Male, Mutation, SARS-CoV-2 genetics, Safety, Vaccination, COVID-19 prevention & control, COVID-19 Vaccines immunology, HIV Infections epidemiology, SARS-CoV-2 immunology

Abstract

Background: People living with HIV are at an increased risk of fatal outcome when admitted to hospital for severe COVID-19 compared with HIV-negative individuals. We aimed to assess safety and immunogenicity of the ChAdOx1 nCoV-19 (AZD1222) vaccine in people with HIV and HIV-negative individuals in South Africa., Methods: In this ongoing, double-blind, placebo-controlled, phase 1B/2A trial (COV005), people with HIV and HIV-negative participants aged 18-65 years were enrolled at seven South African locations and were randomly allocated (1:1) with full allocation concealment to receive a prime-boost regimen of ChAdOx1 nCoV-19, with two doses given 28 days apart. Eligibility criteria for people with HIV included being on antiretroviral therapy for at least 3 months, with a plasma HIV viral load of less than 1000 copies per mL. In this interim analysis, safety and reactogenicity was assessed in all individuals who received at least one dose of ChAdOx1 nCov 19 between enrolment and Jan 15, 2021. Primary immunogenicity analyses included participants who received two doses of trial intervention and were SARS-CoV-2 seronegative at baseline. This trial is registered with ClinicalTrials.gov, NCT04444674, and the Pan African Clinicals Trials Registry, PACTR202006922165132., Findings: Between June 24 and Nov 12, 2020, 104 people with HIV and 70 HIV-negative individuals were enrolled. 102 people with HIV (52 vaccine; 50 placebo) and 56 HIV-negative participants (28 vaccine; 28 placebo) received the priming dose, 100 people with HIV (51 vaccine; 49 placebo) and 46 HIV-negative participants (24 vaccine; 22 placebo) received two doses (priming and booster). In participants seronegative for SARS-CoV-2 at baseline, there were 164 adverse events in those with HIV (86 vaccine; 78 placebo) and 237 in HIV-negative participants (95 vaccine; 142 placebo). Of seven serious adverse events, one severe fever in a HIV-negative participant was definitely related to trial intervention and one severely elevated alanine aminotranferase in a participant with HIV was unlikely related; five others were deemed unrelated. One person with HIV died (unlikely related). People with HIV and HIV-negative participants showed vaccine-induced serum IgG responses against wild-type Wuhan-1 Asp614Gly (also known as D614G). For participants seronegative for SARS-CoV-2 antigens at baseline, full-length spike geometric mean concentration (GMC) at day 28 was 163·7 binding antibody units (BAU)/mL (95% CI 89·9-298·1) for people with HIV (n=36) and 112·3 BAU/mL (61·7-204·4) for HIV-negative participants (n=23), with a rising day 42 GMC booster response in both groups. Baseline SARS-CoV-2 seropositive people with HIV demonstrated higher antibody responses after each vaccine dose than did people with HIV who were seronegative at baseline. High-level binding antibody cross-reactivity for the full-length spike and receptor-binding domain of the beta variant (B.1.351) was seen regardless of HIV status. In people with HIV who developed high titre responses, predominantly those who were receptor-binding domain seropositive at enrolment, neutralising activity against beta was retained., Interpretation: ChAdOx1 nCoV-19 was well tolerated, showing favourable safety and immunogenicity in people with HIV, including heightened immunogenicity in SARS-CoV-2 baseline-seropositive participants. People with HIV showed cross-reactive binding antibodies to the beta variant and Asp614Gly wild-type, and high responders retained neutralisation against beta., Funding: The Bill & Melinda Gates Foundation, South African Medical Research Council, UK Research and Innovation, UK National Institute for Health Research, and the South African Medical Research Council., Competing Interests: Declaration of interests Oxford University has entered into a partnership with AstraZeneca for further development of ChAdOx1 nCoV-19 (AZD1222). AstraZeneca reviewed the data from the trial and the final manuscript before submission, but the authors retained editorial control. SCG is cofounder of Vaccitech, a collaborator in the early development of this vaccine candidate, and is named as an inventor on a patent covering use of ChAdOx1-vectored vaccines (PCT/GB2012/000467) and a patent application covering this SARS-CoV-2 vaccine (GB2003670.3). TL is named as an inventor on a patent application covering ChAdOx1 nCoV-19 and was a consultant to Vaccitech. TLV and JV are employees of AstraZeneca. All other authors declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2021