Your search keyword '"Ryan S. Roark"' showing total 9 results

1. Ultrapotent Broadly Neutralizing Human‐llama Bispecific Antibodies against HIV‐1

Author

Jianliang Xu, Tongqing Zhou, Krisha McKee, Baoshan Zhang, Cuiping Liu, Alexandra F. Nazzari, Amarendra Pegu, Chen‐Hsiang Shen, Jordan E. Becker, Michael F. Bender, Payton Chan, Anita Changela, Ridhi Chaudhary, Xuejun Chen, Tal Einav, Young Do Kwon, Bob C. Lin, Mark K. Louder, Jonah S. Merriam, Nicholas C. Morano, Sijy O'Dell, Adam S. Olia, Reda Rawi, Ryan S. Roark, Tyler Stephens, I‐Ting Teng, Emily Tourtellott‐Fogt, Shuishu Wang, Eun Sung Yang, Lawrence Shapiro, Yaroslav Tsybovsky, Nicole A. Doria‐Rose, Rafael Casellas, and Peter D. Kwong

Subjects

bispecific antibodies, bNAb, broadly neutralizing antibody, HIV‐1, llama, neutralizing nanobodies, Science

Abstract

Abstract Broadly neutralizing antibodies are proposed as therapeutic and prophylactic agents against HIV‐1, but their potency and breadth are less than optimal. This study describes the immunization of a llama with the prefusion‐stabilized HIV‐1 envelope (Env) trimer, BG505 DS‐SOSIP, and the identification and improvement of potent neutralizing nanobodies recognizing the CD4‐binding site (CD4bs) of vulnerability. Two of the vaccine‐elicited CD4bs‐targeting nanobodies, G36 and R27, when engineered into a triple tandem format with llama IgG2a‐hinge region and human IgG1‐constant region (G36×3‐IgG2a and R27×3‐IgG2a), neutralized 96% of a multiclade 208‐strain panel at geometric mean IC80s of 0.314 and 0.033 µg mL−1, respectively. Cryo‐EM structures of these nanobodies in complex with Env trimer revealed the two nanobodies to neutralize HIV‐1 by mimicking the recognition of the CD4 receptor. To enhance their neutralizing potency and breadth, nanobodies are linked to the light chain of the V2‐apex‐targeting broadly neutralizing antibody, CAP256V2LS. The resultant human‐llama bispecific antibody CAP256L‐R27×3LS exhibited ultrapotent neutralization and breadth exceeding other published HIV‐1 broadly neutralizing antibodies, with pharmacokinetics determined in FcRn‐Fc mice similar to the parent CAP256V2LS. Vaccine‐elicited llama nanobodies, when combined with V2‐apex broadly neutralizing antibodies, may therefore be able to fulfill anti‐HIV‐1 therapeutic and prophylactic clinical goals.

Published

2024

2. A Germline-Targeting Chimpanzee SIV Envelope Glycoprotein Elicits a New Class of V2-Apex Directed Cross-Neutralizing Antibodies

Author

Frederic Bibollet-Ruche, Ronnie M. Russell, Wenge Ding, Weimin Liu, Yingying Li, Kshitij Wagh, Daniel Wrapp, Rumi Habib, Ashwin N. Skelly, Ryan S. Roark, Scott Sherrill-Mix, Shuyi Wang, Juliette Rando, Emily Lindemuth, Kendra Cruickshank, Younghoon Park, Rachel Baum, John W. Carey, Andrew Jesse Connell, Hui Li, Elena E. Giorgi, Ge S. Song, Shilei Ding, Andrés Finzi, Amanda Newman, Giovanna E. Hernandez, Emily Machiele, Derek W. Cain, Katayoun Mansouri, Mark G. Lewis, David C. Montefiori, Kevin J. Wiehe, S. Munir Alam, I-Ting Teng, Peter D. Kwong, Raiees Andrabi, Laurent Verkoczy, Dennis R. Burton, Bette T. Korber, Kevin O. Saunders, Barton F. Haynes, Robert J. Edwards, George M. Shaw, and Beatrice H. Hahn

Subjects

SCIV, V2-apex, broadly neutralizing antibodies, chimpanzee, immunofocusing, germline-targeting, Microbiology, QR1-502

Abstract

ABSTRACT HIV-1 and its SIV precursors share a broadly neutralizing antibody (bNAb) epitope in variable loop 2 (V2) at the envelope glycoprotein (Env) trimer apex. Here, we tested the immunogenicity of germ line-targeting versions of a chimpanzee SIV (SIVcpz) Env in human V2-apex bNAb heavy-chain precursor-expressing knock-in mice and as chimeric simian-chimpanzee immunodeficiency viruses (SCIVs) in rhesus macaques (RMs). Trimer immunization of knock-in mice induced V2-directed NAbs, indicating activation of V2-apex bNAb precursor-expressing mouse B cells. SCIV infection of RMs elicited high-titer viremia, potent autologous tier 2 neutralizing antibodies, and rapid sequence escape in the canonical V2-apex epitope. Six of seven animals also developed low-titer heterologous plasma breadth that mapped to the V2-apex. Antibody cloning from two of these animals identified multiple expanded lineages with long heavy chain third complementarity determining regions that cross-neutralized as many as 7 of 19 primary HIV-1 strains, but with low potency. Negative stain electron microscopy (NSEM) of members of the two most cross-reactive lineages confirmed V2 targeting but identified an angle of approach distinct from prototypical V2-apex bNAbs, with antibody binding either requiring or inducing an occluded-open trimer. Probing with conformation-sensitive, nonneutralizing antibodies revealed that SCIV-expressed, but not wild-type SIVcpz Envs, as well as a subset of primary HIV-1 Envs, preferentially adopted a more open trimeric state. These results reveal the existence of a cryptic V2 epitope that is exposed in occluded-open SIVcpz and HIV-1 Env trimers and elicits cross-neutralizing responses of limited breadth and potency. IMPORTANCE An effective HIV-1 vaccination strategy will need to stimulate rare precursor B cells of multiple bNAb lineages and affinity mature them along desired pathways. Here, we searched for V2-apex germ line-targeting Envs among a large set of diverse primate lentiviruses and identified minimally modified versions of one chimpanzee SIV Env that bound several human V2-apex bNAb precursors and stimulated one of these in a V2-apex bNAb precursor-expressing knock-in mouse. We also generated chimeric simian-chimpanzee immunodeficiency viruses and showed that they elicit low-titer V2-directed heterologous plasma breadth in six of seven infected rhesus macaques. Characterization of this antibody response identified a new class of weakly cross-reactive neutralizing antibodies that target the V2-apex, but only in occluded-open Env trimers. The existence of this cryptic epitope, which in some Env backgrounds is immunodominant, needs to be considered in immunogen design.

Published

2023

3. A germline-targeting chimpanzee SIV envelope glycoprotein elicits a new class of V2-apex directed cross-neutralizing antibodies

Author

Frederic Bibollet-Ruche, Ronnie M. Russell, Wenge Ding, Weimin Liu, Yingying Li, Kshitij Wagh, Daniel Wrapp, Rumi Habib, Ashwin N. Skelly, Ryan S. Roark, Scott Sherrill-Mix, Shuyi Wang, Juliette Rando, Emily Lindemuth, Kendra Cruickshank, Younghoon Park, Rachel Baum, Andrew Jesse Connell, Hui Li, Elena E. Giorgi, Ge S. Song, Shilei Ding, Andrés Finzi, Amanda Newman, Giovanna E. Hernandez, Emily Machiele, Derek W. Cain, Katayoun Mansouri, Mark G. Lewis, David C. Montefiori, Kevin J. Wiehe, S. Munir Alam, I-Ting Teng, Peter D. Kwong, Raiees Andrabi, Laurent Verkoczy, Dennis R. Burton, Bette T. Korber, Kevin O. Saunders, Barton F. Haynes, Robert J. Edwards, George M. Shaw, and Beatrice H. Hahn

Abstract

HIV-1 and its SIV precursors share a broadly neutralizing antibody (bNAb) epitope in variable loop 2 (V2) at the envelope glycoprotein (Env) trimer apex. Here, we tested the immunogenicity of germline-targeting versions of a chimpanzee SIV (SIVcpz) Env in human V2-apex bNAb heavy-chain precursor-expressing knock-in mice and as chimeric simian-chimpanzee immunodeficiency viruses (SCIVs) in rhesus macaques (RMs). Trimer immunization of knock-in mice induced V2-directed NAbs, indicating activation of V2-apex bNAb precursor-expressing mouse B cells. SCIV infection of RMs elicited high-titer viremia, potent autologous tier 2 neutralizing antibodies, and rapid sequence escape in the canonical V2-apex epitope. Six of seven animals also developed low-titer heterologous plasma breadth that mapped to the V2-apex. Antibody cloning from two of these identified multiple expanded lineages with long heavy chain third complementarity determining regions that cross-neutralized as many as 7 of 19 primary HIV-1 strains, but with low potency. Negative stain electron microscopy (NSEM) of members of the two most cross-reactive lineages confirmed V2 targeting but identified an angle of approach distinct from prototypical V2-apex bNAbs, with antibody binding either requiring or inducing an occluded-open trimer. Probing with conformation-sensitive, non-neutralizing antibodies revealed that SCIV-expressed Envs as well as some primary HIV-1 Envs adopted a more open conformation, thereby exposing a conserved V2 epitope that is occluded in closed SIVcpz and HIV-1 Env trimers. These results expand the spectrum of V2-apex targeted antibodies that can contribute to neutralization breadth and identify novel SIV Env platforms for further development as germline-targeting and immunofocusing immunogens.One sentence summaryA cryptic V2 epitope in occluded-open HIV and SIV Env trimers is the target of a new class of V2-directed cross-neutralizing antibodies.

Published

2022

4. Mapping Polyclonal HIV-1 Antibody Responses via Next-Generation Neutralization Fingerprinting.

Author

Nicole A Doria-Rose, Han R Altae-Tran, Ryan S Roark, Stephen D Schmidt, Matthew S Sutton, Mark K Louder, Gwo-Yu Chuang, Robert T Bailer, Valerie Cortez, Rui Kong, Krisha McKee, Sijy O'Dell, Felicia Wang, Salim S Abdool Karim, James M Binley, Mark Connors, Barton F Haynes, Malcolm A Martin, David C Montefiori, Lynn Morris, Julie Overbaugh, Peter D Kwong, John R Mascola, and Ivelin S Georgiev

Subjects

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

Abstract

Computational neutralization fingerprinting, NFP, is an efficient and accurate method for predicting the epitope specificities of polyclonal antibody responses to HIV-1 infection. Here, we present next-generation NFP algorithms that substantially improve prediction accuracy for individual donors and enable serologic analysis for entire cohorts. Specifically, we developed algorithms for: (a) selection of optimized virus neutralization panels for NFP analysis, (b) estimation of NFP prediction confidence for each serum sample, and (c) identification of sera with potentially novel epitope specificities. At the individual donor level, the next-generation NFP algorithms particularly improved the ability to detect multiple epitope specificities in a sample, as confirmed both for computationally simulated polyclonal sera and for samples from HIV-infected donors. Specifically, the next-generation NFP algorithms detected multiple specificities in twice as many samples of simulated sera. Further, unlike the first-generation NFP, the new algorithms were able to detect both of the previously confirmed antibody specificities, VRC01-like and PG9-like, in donor CHAVI 0219. At the cohort level, analysis of ~150 broadly neutralizing HIV-infected donor samples suggested a potential connection between clade of infection and types of elicited epitope specificities. Most notably, while 10E8-like antibodies were observed in infections from different clades, an enrichment of such antibodies was predicted for clade B samples. Ultimately, such large-scale analyses of antibody responses to HIV-1 infection can help guide the design of epitope-specific vaccines that are tailored to take into account the prevalence of infecting clades within a specific geographic region. Overall, the next-generation NFP technology will be an important tool for the analysis of broadly neutralizing polyclonal antibody responses against HIV-1.

Published

2017

5. New SHIVs and Improved Design Strategy for Modeling HIV-1 Transmission, Immunopathogenesis, Prevention and Cure

Author

Beatrice H. Hahn, Jessica G. Smith, Yu Ding, Neha Chohan, Brandon F. Keele, Mark G. Lewis, Katharine J. Bar, Alex I. Murphy, Cristian Apetrei, Jeffrey D. Lifson, Hui Li, Fang-Hua Lee, Ivona Pandrea, Thomas N. Denny, Barton F. Haynes, Emily Lindemuth, Juliette Rando, Shuyi Wang, Chengyan Zhao, George M. Shaw, Ryan S. Roark, and Eunlim Kim

Subjects

Antigenicity, simian immunodeficiency virus, viruses, animal diseases, Immunology, Biology, Gp41, Microbiology, Virus, Neutralization, 03 medical and health sciences, 0302 clinical medicine, In vivo, Viral entry, Virology, Gene, Tropism, 030304 developmental biology, 0303 health sciences, human immunodeficiency virus, Wild type, virus diseases, Vaccine efficacy, In vitro, AIDS, Immunization, SHIV, Insect Science, biology.protein, Pathogenesis and Immunity, Antibody, 030217 neurology & neurosurgery

Abstract

SHIV infection of Indian rhesus macaques is an important animal model for studying HIV-1 transmission, prevention, immunopathogenesis, and cure. Such research is timely, given recent progress with active and passive immunization and novel approaches to HIV-1 cure., Previously, we showed that substitution of HIV-1 envelope (Env) residue 375-Ser by bulky aromatic residues enhances binding to rhesus CD4 and enables primary HIV-1 Envs to support efficient replication as simian-human immunodeficiency virus (SHIV) chimeras in rhesus macaques (RMs). Here, we test this design strategy more broadly by constructing SHIVs containing 10 primary Envs corresponding to HIV-1 subtypes A, B, C, AE, and AG. All 10 SHIVs bearing wild-type Env375 residues replicated efficiently in human CD4+ T cells, but only one replicated efficiently in primary rhesus cells. This was a subtype AE SHIV that naturally contained His at Env375. Replacement of wild-type Env375 residues by Trp, Tyr, Phe, or His in the other nine SHIVs led to efficient replication in rhesus CD4+ T cells in vitro and in vivo. Nine SHIVs containing optimized Env375 alleles were grown large-scale in primary rhesus CD4+ T cells to serve as challenge stocks in preclinical prevention trials. These virus stocks were genetically homogeneous, native-like in Env antigenicity and tier 2 neutralization sensitivity, and transmissible by rectal, vaginal, penile, oral, or intravenous routes. To facilitate future SHIV constructions, we engineered a simplified second-generation design scheme and validated it in RMs. Overall, our findings demonstrate that SHIVs bearing primary Envs with bulky aromatic substitutions at Env375 consistently replicate in RMs, recapitulating many features of HIV-1 infection in humans. Such SHIVs are efficiently transmitted by mucosal routes common to HIV-1 infection and can be used to test vaccine efficacy in preclinical monkey trials. IMPORTANCE SHIV infection of Indian rhesus macaques is an important animal model for studying HIV-1 transmission, prevention, immunopathogenesis, and cure. Such research is timely, given recent progress with active and passive immunization and novel approaches to HIV-1 cure. Given the multifaceted roles of HIV-1 Env in cell tropism and virus entry, and as a target for neutralizing and nonneutralizing antibodies, Envs selected for SHIV construction are of paramount importance. Until recently, it has been impossible to strategically design SHIVs bearing clinically relevant Envs that replicate consistently in monkeys. This changed with the discovery that bulky aromatic substitutions at residue Env375 confer enhanced affinity to rhesus CD4. Here, we show that 10 new SHIVs bearing primary HIV-1 Envs with residue 375 substitutions replicated efficiently in RMs and could be transmitted efficiently across rectal, vaginal, penile, and oral mucosa. These findings suggest an expanded role for SHIVs as a model of HIV-1 infection.

Published

2021

6. Recapitulation of HIV-1 Env-Antibody Coevolution in Macaques Leading to Neutralization Breadth

Author

Shuyi Wang, Chengyan Zhao, Anya M. Bauer, Fang-Hua Lee, Cara W. Chao, Emily Lindemuth, Nicole A. Doria-Rose, Juliette Rando, Frederic Bibollet-Ruche, Kevin Wiehe, Mario Roederer, Chaim A. Schramm, Bette T. Korber, Donald D. Raymond, Kwan-Ki Hwang, Weimin Liu, George M. Shaw, Mark G. Lewis, Ronnie M. Russell, Hui Li, Stephen C. Harrison, Baoshan Zhang, Ryan S. Roark, Andrew G. Smith, Jesse Connell, Kevin O. Saunders, Hui Geng, Alexander I. Murphy, Mattia Bonsignori, Elena E. Giorgi, Maho Okumura, Hema Chug, Beatrice H. Hahn, John R. Mascola, Peter D. Kwong, Peter T. Hraber, Christina Rosario, Jessica G. Smith, David R. Ambrozak, Yu Ding, Wenge Ding, Richard Nguyen, Rosemarie D. Mason, Barton F. Haynes, Mark K. Louder, Daniel C. Douek, Kshitij Wagh, Jason Gorman, Bob C. Lin, Thomas B. Kepler, Wilton B. Williams, Neha Chohan, Garnett Kelsoe, Gwo-Yu Chuang, Julia DeVoto, Katharine J. Bar, and M. Anthony Moody

Subjects

0301 basic medicine, Immunogen, viruses, Human immunodeficiency virus (HIV), HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Biology, Virus Replication, medicine.disease_cause, Article, Epitope, Neutralization, Biological Coevolution, Epitopes, 03 medical and health sciences, 0302 clinical medicine, Viral envelope, medicine, Animals, Humans, Binding site, Immunodeficiency, Coevolution, Binding Sites, Multidisciplinary, Cryoelectron Microscopy, Molecular Mimicry, virus diseases, medicine.disease, Macaca mulatta, Virology, 030104 developmental biology, Viral replication, CD4 Antigens, HIV-1, biology.protein, Simian Immunodeficiency Virus, Antibody, Viral persistence, Broadly Neutralizing Antibodies, 030217 neurology & neurosurgery

Abstract

Convergent HIV evolution across species Human immunodeficiency virus (HIV) has a highly diverse envelope protein that it uses to target human cells, and the complexity of the viral envelope has stymied vaccine development. Roark et al. report that the immediate and short-term evolutionary potential of the HIV envelope is constrained because of a number of essential functions, including antibody escape. Consequently, when introduced into humans as HIV or into rhesus macaque monkeys as chimeric simian-human immunodeficiency virus, homologous envelope glycoproteins appear to exhibit conserved patterns of sequence evolution, in some cases eliciting broadly neutralizing antibodies in both hosts. Conserved patterns of envelope variation and homologous B cell responses in humans and monkeys represent examples of convergent evolution that may serve to guide HIV vaccine development. Science , this issue p. eabd2638

Published

2020

7. New Member of the V1V2-Directed CAP256-VRC26 Lineage That Shows Increased Breadth and Exceptional Potency

Author

Marie Pancera, Mark K. Louder, Stephen D. Schmidt, Matthew S. Sutton, Lawrence Shapiro, Peter D. Kwong, Jinal N. Bhiman, Amarendra Pegu, Mangaiarkarasi Asokan, Penny L. Moore, Robert T. Bailer, Ryan P. Staupe, Sijy O'Dell, John R. Mascola, Salim Abdool-Karim, Chaim A. Schramm, Evan M. Cale, Lynn Morris, Marissa C. Jarosinski, Rebecca M. Lynch, Keyun Wang, Jason Gorman, Nicole A. Doria-Rose, Gwo-Yu Chuang, Aliaksandr Druz, Krisha McKee, Constantinos Kurt Wibmer, Barton F. Haynes, Nigel Garrett, Isabella R. Fraschilla, Ryan S. Roark, and Michael J. Ernandes

Subjects

0301 basic medicine, Glycan, Lineage (genetic), Molecular Sequence Data, Immunology, HIV Infections, Cross Reactions, HIV Antibodies, HIV Envelope Protein gp120, Microbiology, Neutralization, Epitope, Inhibitory Concentration 50, 03 medical and health sciences, Virology, Humans, Potency, Clade, biology, Sequence Analysis, DNA, Antibodies, Neutralizing, 030104 developmental biology, Epitope mapping, Insect Science, HIV-1, biology.protein, Pathogenesis and Immunity, Female, Antibody, Epitope Mapping

Abstract

The epitopes defined by HIV-1 broadly neutralizing antibodies (bNAbs) are valuable templates for vaccine design, and studies of the immunological development of these antibodies are providing insights for vaccination strategies. In addition, the most potent and broadly reactive of these bNAbs have potential for clinical use. We previously described a family of 12 V1V2-directed neutralizing antibodies, CAP256-VRC26, isolated from an HIV-1 clade C-infected donor at years 1, 2, and 4 of infection (N. A. Doria-Rose et al., Nature 509:55–62, 2014, http://dx.doi.org/10.1038/nature13036 ). Here, we report on the isolation and characterization of new members of the family mostly obtained at time points of peak serum neutralization breadth and potency. Thirteen antibodies were isolated from B cell culture, and eight were isolated using trimeric envelope probes for differential single B cell sorting. One of the new antibodies displayed a 10-fold greater neutralization potency than previously published lineage members. This antibody, CAP256-VRC26.25, neutralized 57% of diverse clade viral isolates and 70% of clade C isolates with remarkable potency. Among the viruses neutralized, the median 50% inhibitory concentration was 0.001 μg/ml. All 33 lineage members targeted a quaternary epitope focused on V2. While all known bNAbs targeting the V1V2 region interact with the N160 glycan, the CAP256-VRC26 antibodies showed an inverse correlation of neutralization potency with dependence on this glycan. Overall, our results highlight the ongoing evolution within a single antibody lineage and describe more potent and broadly neutralizing members with potential clinical utility, particularly in areas where clade C is prevalent. IMPORTANCE Studies of HIV-1 broadly neutralizing antibodies (bNAbs) provide valuable information for vaccine design, and the most potent and broadly reactive of these bNAbs have potential for clinical use. We previously described a family of V1V2-directed neutralizing antibodies from an HIV-1 clade C-infected donor. Here, we report on the isolation and characterization of new members of the family mostly obtained at time points of peak serum neutralization breadth and potency. One of the new antibodies, CAP256-VRC26.25, displayed a 10-fold greater neutralization potency than previously described lineage members. It neutralized 57% of diverse clade viral isolates and 70% of clade C isolates with remarkable potency: the median 50% inhibitory concentration was 0.001 μg/ml. Our results highlight the ongoing evolution within a single antibody lineage and describe more potent and broadly neutralizing members with potential clinical utility, particularly in areas where clade C is prevalent.

Published

2016

8. Mapping Polyclonal HIV-1 Antibody Responses via Next-Generation Neutralization Fingerprinting

Author

Mark K. Louder, Ryan S. Roark, Nicole A. Doria-Rose, Valerie Cortez, Stephen D. Schmidt, James M. Binley, David C. Montefiori, Rui Kong, Julie Overbaugh, Malcolm A. Martin, Krisha McKee, Ivelin S. Georgiev, Peter D. Kwong, Han Altae-Tran, Lynn Morris, Robert T. Bailer, Sijy O'Dell, Gwo-Yu Chuang, John R. Mascola, Mark Connors, Matthew S. Sutton, Salim S. Abdool Karim, Barton F. Haynes, Felicia. Wang, and Trkola, Alexandra

Subjects

0301 basic medicine, RNA viruses, Physiology, Antibody Response, HIV Infections, HIV Antibodies, Pathology and Laboratory Medicine, Biochemistry, Epitope, Neutralization, Serology, Cohort Studies, Epitopes, Immunodeficiency Viruses, Antibody Specificity, Immune Physiology, Medicine and Health Sciences, Clade, lcsh:QH301-705.5, Immune Response, AIDS Vaccines, Immune System Proteins, Applied Mathematics, Simulation and Modeling, 3. Good health, Infectious Diseases, Medical Microbiology, Viral Pathogens, Viruses, Physical Sciences, HIV/AIDS, Antibody, Pathogens, Infection, Algorithms, Research Article, lcsh:Immunologic diseases. Allergy, Optimization, medicine.drug_class, 030106 microbiology, Immunology, Biology, Monoclonal antibody, Research and Analysis Methods, Microbiology, Antibodies, Vaccine Related, 03 medical and health sciences, Neutralization Tests, Virology, Retroviruses, Genetics, medicine, Humans, Computer Simulation, Vaccine Related (AIDS), Molecular Biology, Microbial Pathogens, Prevention, Lentivirus, Organisms, Biology and Life Sciences, Proteins, HIV, Monoclonal Antibodies, Good Health and Well Being, 030104 developmental biology, Antibody response, lcsh:Biology (General), Polyclonal antibodies, Antibody Formation, biology.protein, HIV-1, Immunization, Parasitology, lcsh:RC581-607, Mathematics, Epitope Mapping

Abstract

Computational neutralization fingerprinting, NFP, is an efficient and accurate method for predicting the epitope specificities of polyclonal antibody responses to HIV-1 infection. Here, we present next-generation NFP algorithms that substantially improve prediction accuracy for individual donors and enable serologic analysis for entire cohorts. Specifically, we developed algorithms for: (a) selection of optimized virus neutralization panels for NFP analysis, (b) estimation of NFP prediction confidence for each serum sample, and (c) identification of sera with potentially novel epitope specificities. At the individual donor level, the next-generation NFP algorithms particularly improved the ability to detect multiple epitope specificities in a sample, as confirmed both for computationally simulated polyclonal sera and for samples from HIV-infected donors. Specifically, the next-generation NFP algorithms detected multiple specificities in twice as many samples of simulated sera. Further, unlike the first-generation NFP, the new algorithms were able to detect both of the previously confirmed antibody specificities, VRC01-like and PG9-like, in donor CHAVI 0219. At the cohort level, analysis of ~150 broadly neutralizing HIV-infected donor samples suggested a potential connection between clade of infection and types of elicited epitope specificities. Most notably, while 10E8-like antibodies were observed in infections from different clades, an enrichment of such antibodies was predicted for clade B samples. Ultimately, such large-scale analyses of antibody responses to HIV-1 infection can help guide the design of epitope-specific vaccines that are tailored to take into account the prevalence of infecting clades within a specific geographic region. Overall, the next-generation NFP technology will be an important tool for the analysis of broadly neutralizing polyclonal antibody responses against HIV-1., Author Summary HIV-1 remains a significant global health threat, with no effective vaccine against the virus currently available. Since traditional vaccine design efforts have had limited success, much effort in recent years has focused on gaining a better understanding of the ways select individuals are able to effectively neutralize the virus upon natural infection, and to utilize that knowledge for the design of optimized vaccine candidates. Primary emphasis has been placed on characterizing the antibody arm of the immune system, and specifically on antibodies capable of neutralizing the majority of circulating HIV-1 strains. Various experimental techniques can be applied to map the epitope targets of these antibodies, but more recently, the development of computational methods has provided an efficient and accurate alternative for understanding the complex antibody responses to HIV-1 in a given individual. Here, we present the next generation of this computational technology, and show that these new methods have significantly improved accuracy and confidence, and that they enable the interrogation of biologically important questions that can lead to new insights for the design of an effective vaccine against HIV-1.

Published

2017

9. Variable Dependence on Glycan Recognition within a Lineage of V1V2-directed HIV Neutralizing Antibodies

Author

Ryan S. Roark, Jinal N. Bhiman, Michael J. Ernandes, Krisha McKee, Mark K. Louder, John R. Mascola, Lawrence Shapiro, Lynn Morris, Salim S. Abdool Karim, Chaim A. Schramm, Penny L. Moore, Nicole A. Doria-Rose, and Sijy O'Dell

Subjects

Tyrosine sulfation, Glycan, Lineage (genetic), biology, Immunology, Virology, Glycans and Antibody Effector Functions, Neutralization, Virus, Epitope, Infectious Diseases, medicine.anatomical_structure, biology.protein, medicine, Antibody, B cell

Abstract

PD05.02 Background: The study of HIV donors with broad and potent neutralizing antibodies can inform rational vaccine design and immunization strategies. We previously identified 12 antibodies from a single lineage in donor CAP256 that target V1V2 with breadth up to 60% in clades A and C, and very high potency on many strains. The antibodies varied in dependence on glycan. We sought to isolate additional lineage members and to understand variation in epitope recognition. Methods: Antibodies were isolated via 14-day B cell culture with IL-2, IL-21, and CD40L. Initial RTPCR was performed using IgG-specific primers. For weeks 119 and 206, wells were re-interrogated using IgA-specific primers. 5 additional antibodies were isolated from week 119 and 4 from week 206, and reconstituted as IgG1 and IgA1. The IgGs were assayed for neutralization on TZM-bl cells on a panel of 49 autologous and heterologous Env-pseudoviruses, as well as viruses with mutations in known epitopes. Results: Several B cell culture wells yielded both IgG and IgA amplicons with the same VDJ sequence, suggesting that class-switching occurred during culture. Nine new antibodies of the CAP256-VRC26 lineage were identified, several of which had breadth similar to the previous best members of the lineage. Two from week 206 lack the characteristic tyrosine sulfation signal, and are also less broadly neutralizing. All depend on residues in V2, with variable and strain-specific effects of glycans. We examined the impact of removing the glycan at N160 which is critical for the PG9 class: some lost neutralization; some were unaffected; and CAP256-VRC26.13, and two nearly identical antibodies cloned independently, showed gain of neutralization, the opposite of PG9. Conclusions: We have expanded the CAP256-VRC26 clonal family. Its members show diversity in recognition of specific determinants within the V1V2 epitope, particularly the glycans, which vary in the virus as a means of escape from antibody pressure.

Published

2014