Your search keyword '"Chen-Hsiang Shen"' showing total 72 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. Cleavage-intermediate Lassa virus trimer elicits neutralizing responses, identifies neutralizing nanobodies, and reveals an apex-situated site-of-vulnerability

Author

Jason Gorman, Crystal Sao-Fong Cheung, Zhijian Duan, Li Ou, Maple Wang, Xuejun Chen, Cheng Cheng, Andrea Biju, Yaping Sun, Pengfei Wang, Yongping Yang, Baoshan Zhang, Jeffrey C. Boyington, Tatsiana Bylund, Sam Charaf, Steven J. Chen, Haijuan Du, Amy R. Henry, Tracy Liu, Edward K. Sarfo, Chaim A. Schramm, Chen-Hsiang Shen, Tyler Stephens, I-Ting Teng, John-Paul Todd, Yaroslav Tsybovsky, Raffaello Verardi, Danyi Wang, Shuishu Wang, Zhantong Wang, Cheng-Yan Zheng, Tongqing Zhou, Daniel C. Douek, John R. Mascola, David D. Ho, Mitchell Ho, and Peter D. Kwong

Subjects

Science

Abstract

Abstract Lassa virus (LASV) infection is expanding outside its traditionally endemic areas in West Africa, posing a pandemic biothreat. LASV-neutralizing antibodies, moreover, have proven difficult to elicit. To gain insight into LASV neutralization, here we develop a prefusion-stabilized LASV glycoprotein trimer (GPC), pan it against phage libraries comprising single-domain antibodies (nanobodies) from shark and camel, and identify one, D5, which neutralizes LASV. Cryo-EM analyses reveal D5 to recognize a cleavage-dependent site-of-vulnerability at the trimer apex. The recognized site appears specific to GPC intermediates, with protomers lacking full cleavage between GP1 and GP2 subunits. Guinea pig immunizations with the prefusion-stabilized cleavage-intermediate LASV GPC, first as trimer and then as a nanoparticle, induce neutralizing responses, targeting multiple epitopes including that of D5; we identify a neutralizing antibody (GP23) from the immunized guinea pigs. Collectively, our findings define a prefusion-stabilized GPC trimer, reveal an apex-situated site-of-vulnerability, and demonstrate elicitation of LASV-neutralizing responses by a cleavage-intermediate LASV trimer.

Published

2024

3. Antibody-directed evolution reveals a mechanism for enhanced neutralization at the HIV-1 fusion peptide site

Author

Bailey B. Banach, Sergei Pletnev, Adam S. Olia, Kai Xu, Baoshan Zhang, Reda Rawi, Tatsiana Bylund, Nicole A. Doria-Rose, Thuy Duong Nguyen, Ahmed S. Fahad, Myungjin Lee, Bob C. Lin, Tracy Liu, Mark K. Louder, Bharat Madan, Krisha McKee, Sijy O’Dell, Mallika Sastry, Arne Schön, Natalie Bui, Chen-Hsiang Shen, Jacy R. Wolfe, Gwo-Yu Chuang, John R. Mascola, Peter D. Kwong, and Brandon J. DeKosky

Subjects

Science

Abstract

Abstract The HIV-1 fusion peptide (FP) represents a promising vaccine target, but global FP sequence diversity among circulating strains has limited anti-FP antibodies to ~60% neutralization breadth. Here we evolve the FP-targeting antibody VRC34.01 in vitro to enhance FP-neutralization using site saturation mutagenesis and yeast display. Successive rounds of directed evolution by iterative selection of antibodies for binding to resistant HIV-1 strains establish a variant, VRC34.01_mm28, as a best-in-class antibody with 10-fold enhanced potency compared to the template antibody and ~80% breadth on a cross-clade 208-strain neutralization panel. Structural analyses demonstrate that the improved paratope expands the FP binding groove to accommodate diverse FP sequences of different lengths while also recognizing the HIV-1 Env backbone. These data reveal critical antibody features for enhanced neutralization breadth and potency against the FP site of vulnerability and accelerate clinical development of broad HIV-1 FP-targeting vaccines and therapeutics.

Published

2023

4. High frequency of HIV precursor-target-specific B cells in sub-Saharan populations

Author

Flavio Matassoli, Alberto Cagigi, Chen-Hsiang Shen, Amy R. Henry, Timothy S. Johnston, Chaim A. Schramm, Christopher A. Cottrell, Oleksandr Kalyuzhniy, Abby Spangler, Leigh Eller, Merlin Robb, Michael Eller, Prossy Naluyima, Peter D. Kwong, Daniel C. Douek, William R. Schief, Sarah F. Andrews, and Adrian B. McDermott

Subjects

CP: Immunology, CP: Microbiology, Biology (General), QH301-705.5

Abstract

Summary: HIV gp120 engineered outer domain germline-targeting version 8 (eOD-GT8) was designed specifically to engage naive B cell precursors of VRC01-class antibodies. However, the frequency and affinity of naive B cell precursors able to recognize eOD-GT8 have been evaluated only in U.S. populations. HIV infection is disproportionally concentrated in sub-Saharan Africa, so we seek to characterize naive B cells able to recognize eOD-GT8 in sub-Saharan cohorts. We demonstrate that people from sub-Saharan Africa have a higher or equivalent frequency of naive B cells able to engage eOD-GT8 compared with people from the U.S. Genetically, the higher frequency of eOD-GT8-positive cells is accompanied by a higher level of naive B cells with gene signatures characteristic of the VRC01 class, as well as other CD4bs-directed antibodies. Our study demonstrates that vaccination with eOD-GT8 in sub-Saharan Africa could be successful at expanding and establishing a pool of CD4bs-directed memory B cells from naive precursors.

Published

2023

5. Improved pharmacokinetics of HIV-neutralizing VRC01-class antibodies achieved by reduction of net positive charge on variable domain

Author

Young D. Kwon, Amarendra Pegu, Eun Sung Yang, Baoshan Zhang, Michael F. Bender, Mangaiarkarasi Asokan, Qingbo Liu, Krisha McKee, Bob C. Lin, Tracy Liu, Mark K. Louder, Reda Rawi, Mateo Reveiz, Andrew J. Schaub, Chen-Hsiang Shen, Nicole A. Doria-Rose, Paolo Lusso, John R. Mascola, and Peter D. Kwong

Subjects

Antibody-mediated prevention, net positive charge reduction, pharmacokinetics, serum half-life, surface charge, variable region, Therapeutics. Pharmacology, RM1-950, Immunologic diseases. Allergy, RC581-607

Abstract

ABSTRACTThe amino-acid composition of the immunoglobulin variable region has been observed to impact antibody pharmacokinetics (PK). Here, we sought to improve the PK of the broad HIV−1-neutralizing VRC01-class antibodies, VRC07-523LS and N6LS, by reducing the net positive charge in their variable domains. We used a structure-guided approach to generate a panel of antibody variants incorporating select Arg or Lys substituted to Asp, Gln, Glu, or Ser. The engineered variants exhibited reduced affinity to heparin, reduced polyreactivity, and improved PK in human FcRn-transgenic mice. One variant, VRC07-523LS.v34, with three charge substitutions, had an observed in vivo half-life and an estimated human half-life of 10.8 and 60 days, respectively (versus 5.4 and 38 days for VRC07-523LS) and retained functionality, neutralizing 92% of a 208-strain panel at a geometric mean IC80

Published

2023

6. Engineering of HIV-1 neutralizing antibody CAP256V2LS for manufacturability and improved half life

Author

Baoshan Zhang, Deepika Gollapudi, Jason Gorman, Sijy O’Dell, Leland F. Damron, Krisha McKee, Mangaiarkarasi Asokan, Eun Sung Yang, Amarendra Pegu, Bob C. Lin, Cara W. Chao, Xuejun Chen, Lucio Gama, Vera B. Ivleva, William H. Law, Cuiping Liu, Mark K. Louder, Stephen D. Schmidt, Chen-Hsiang Shen, Wei Shi, Judith A. Stein, Michael S. Seaman, Adrian B. McDermott, Kevin Carlton, John R. Mascola, Peter D. Kwong, Q. Paula Lei, and Nicole A. Doria-Rose

Subjects

Medicine, Science

Abstract

Abstract The broadly neutralizing antibody (bNAb) CAP256-VRC26.25 has exceptional potency against HIV-1 and has been considered for clinical use. During the characterization and production of this bNAb, we observed several unusual features. First, the antibody appeared to adhere to pipette tips, requiring tips to be changed during serial dilution to accurately measure potency. Second, during production scale-up, proteolytic cleavage was discovered to target an extended heavy chain loop, which was attributed to a protease in spent medium from 2-week culture. To enable large scale production, we altered the site of cleavage via a single amino acid change, K100mA. The resultant antibody retained potency and breadth while avoiding protease cleavage. We also added the half-life extending mutation LS, which improved the in vivo persistence in animal models, but did not impact neutralization activity; we observed the same preservation of neutralization for bNAbs VRC01, N6, and PGDM1400 with LS on a 208-virus panel. The final engineered antibody, CAP256V2LS, retained the extraordinary neutralization potency of the parental antibody, had a favorable pharmacokinetic profile in animal models, and was negative in in vitro assessment of autoreactivity. CAP256V2LS has the requisite potency, developability and suitability for scale-up, allowing its advancement as a clinical candidate.

Published

2022

7. Improved HIV-1 neutralization breadth and potency of V2-apex antibodies by in silico design

Author

Graham T. Holt, Jason Gorman, Siyu Wang, Anna U. Lowegard, Baoshan Zhang, Tracy Liu, Bob C. Lin, Mark K. Louder, Marcel S. Frenkel, Krisha McKee, Sijy O’Dell, Reda Rawi, Chen-Hsiang Shen, Nicole A. Doria-Rose, Peter D. Kwong, and Bruce R. Donald

Subjects

CP: Microbiology, CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: Broadly neutralizing antibodies (bNAbs) against HIV can reduce viral transmission in humans, but an effective therapeutic will require unusually high breadth and potency of neutralization. We employ the OSPREY computational protein design software to engineer variants of two apex-directed bNAbs, PGT145 and PG9RSH, resulting in increases in potency of over 100-fold against some viruses. The top designed variants improve neutralization breadth from 39% to 54% at clinically relevant concentrations (IC80

Published

2023

8. HIV-1 neutralizing antibodies elicited in humans by a prefusion-stabilized envelope trimer form a reproducible class targeting fusion peptide

Author

Shuishu Wang, Flavio Matassoli, Baoshan Zhang, Tracy Liu, Chen-Hsiang Shen, Tatsiana Bylund, Timothy Johnston, Amy R. Henry, I-Ting Teng, Prabhanshu Tripathi, Jordan E. Becker, Anita Changela, Ridhi Chaudhary, Cheng Cheng, Martin Gaudinski, Jason Gorman, Darcy R. Harris, Myungjin Lee, Nicholas C. Morano, Laura Novik, Sijy O’Dell, Adam S. Olia, Danealle K. Parchment, Reda Rawi, Jesmine Roberts-Torres, Tyler Stephens, Yaroslav Tsybovsky, Danyi Wang, David J. Van Wazer, Tongqing Zhou, Nicole A. Doria-Rose, Richard A. Koup, Lawrence Shapiro, Daniel C. Douek, Adrian B. McDermott, and Peter D. Kwong

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: Elicitation of antibodies that neutralize the tier-2 neutralization-resistant isolates that typify HIV-1 transmission has been a long-sought goal. Success with prefusion-stabilized envelope trimers eliciting autologous neutralizing antibodies has been reported in multiple vaccine-test species, though not in humans. To investigate elicitation of HIV-1 neutralizing antibodies in humans, here, we analyze B cells from a phase I clinical trial of the “DS-SOSIP”-stabilized envelope trimer from strain BG505, identifying two antibodies, N751-2C06.01 and N751-2C09.01 (named for donor-lineage.clone), that neutralize the autologous tier-2 strain, BG505. Though derived from distinct lineages, these antibodies form a reproducible antibody class that targets the HIV-1 fusion peptide. Both antibodies are highly strain specific, which we attribute to their partial recognition of a BG505-specific glycan hole and to their binding requirements for a few BG505-specific residues. Prefusion-stabilized envelope trimers can thus elicit autologous tier-2 neutralizing antibodies in humans, with initially identified neutralizing antibodies recognizing the fusion-peptide site of vulnerability.

Published

2023

9. Structural basis of LAIR1 targeting by polymorphic Plasmodium RIFINs

Author

Kai Xu, Yiran Wang, Chen-Hsiang Shen, Yiwei Chen, Baoshan Zhang, Kevin Liu, Yaroslav Tsybovsky, Shuishu Wang, S. Katie Farney, Jason Gorman, Tyler Stephens, Raffaello Verardi, Yongping Yang, Tongqing Zhou, Gwo-Yu Chuang, Antonio Lanzavecchia, Luca Piccoli, and Peter D. Kwong

Subjects

Science

Abstract

RIFINs are Plasmodium surface antigens that suppress the immune response by binding inhibitory receptors such as LAIR1. Here, Xu et al. characterize the interaction between RIFIN-variable 2 domain and a LAIR1 domain and identify LAIR1-binding RIFINs in several Plasmodium species.

Published

2021

10. Structural basis of glycan276-dependent recognition by HIV-1 broadly neutralizing antibodies

Author

Christopher A. Cottrell, Kartik Manne, Rui Kong, Shuishu Wang, Tongqing Zhou, Gwo-Yu Chuang, Robert J. Edwards, Rory Henderson, Katarzyna Janowska, Megan Kopp, Bob C. Lin, Mark K. Louder, Adam S. Olia, Reda Rawi, Chen-Hsiang Shen, Justin D. Taft, Jonathan L. Torres, Nelson R. Wu, Baoshan Zhang, Nicole A. Doria-Rose, Myron S. Cohen, Barton F. Haynes, Lawrence Shapiro, Andrew B. Ward, Priyamvada Acharya, John R. Mascola, and Peter D. Kwong

Subjects

antibody-antigen binding, antibody approach angle, CD4 binding site, cryo-EM, glycan conformation, glycan276, Biology (General), QH301-705.5

Abstract

Summary: Recognition of N-linked glycan at residue N276 (glycan276) at the periphery of the CD4-binding site (CD4bs) on the HIV-envelope trimer is a formidable challenge for many CD4bs-directed antibodies. To understand how this glycan can be recognized, here we isolate two lineages of glycan276-dependent CD4bs antibodies. Antibody CH540-VRC40.01 (named for donor-lineage.clone) neutralizes 81% of a panel of 208 diverse strains, while antibody CH314-VRC33.01 neutralizes 45%. Cryo-electron microscopy (cryo-EM) structures of these two antibodies and 179NC75, a previously identified glycan276-dependent CD4bs antibody, in complex with HIV-envelope trimer reveal substantially different modes of glycan276 recognition. Despite these differences, binding of glycan276-dependent antibodies maintains a glycan276 conformation similar to that observed in the absence of glycan276-binding antibodies. By contrast, glycan276-independent CD4bs antibodies, such as VRC01, displace glycan276 upon binding. These results provide a foundation for understanding antibody recognition of glycan276 and suggest its presence may be crucial for priming immunogens seeking to initiate broad CD4bs recognition.

Published

2021

11. Paired heavy- and light-chain signatures contribute to potent SARS-CoV-2 neutralization in public antibody responses

Author

Bailey B. Banach, Gabriele Cerutti, Ahmed S. Fahad, Chen-Hsiang Shen, Matheus Oliveira De Souza, Phinikoula S. Katsamba, Yaroslav Tsybovsky, Pengfei Wang, Manoj S. Nair, Yaoxing Huang, Irene M. Francino-Urdániz, Paul J. Steiner, Matías Gutiérrez-González, Lihong Liu, Sheila N. López Acevedo, Alexandra F. Nazzari, Jacy R. Wolfe, Yang Luo, Adam S. Olia, I-Ting Teng, Jian Yu, Tongqing Zhou, Eswar R. Reddem, Jude Bimela, Xiaoli Pan, Bharat Madan, Amy D. Laflin, Rajani Nimrania, Kwok-Yung Yuen, Timothy A. Whitehead, David D. Ho, Peter D. Kwong, Lawrence Shapiro, and Brandon J. DeKosky

Subjects

SARS-CoV-2, public antibody, neutralization, yeast display, B-cell, biotechnology, Biology (General), QH301-705.5

Abstract

Summary: Understanding mechanisms of protective antibody recognition can inform vaccine and therapeutic strategies against SARS-CoV-2. We report a monoclonal antibody, 910-30, targeting the SARS-CoV-2 receptor-binding site for ACE2 as a member of a public antibody response encoded by IGHV3-53/IGHV3-66 genes. Sequence and structural analyses of 910-30 and related antibodies explore how class recognition features correlate with SARS-CoV-2 neutralization. Cryo-EM structures of 910-30 bound to the SARS-CoV-2 spike trimer reveal binding interactions and its ability to disassemble spike. Despite heavy-chain sequence similarity, biophysical analyses of IGHV3-53/3-66-encoded antibodies highlight the importance of native heavy:light pairings for ACE2-binding competition and SARS-CoV-2 neutralization. We develop paired heavy:light class sequence signatures and determine antibody precursor prevalence to be ∼1 in 44,000 human B cells, consistent with public antibody identification in several convalescent COVID-19 patients. These class signatures reveal genetic, structural, and functional immune features that are helpful in accelerating antibody-based medical interventions for SARS-CoV-2.

Published

2021

12. Improvement of antibody functionality by structure-guided paratope engraftment

Author

Qingbo Liu, Yen-Ting Lai, Peng Zhang, Mark K. Louder, Amarendra Pegu, Reda Rawi, Mangaiarkarasi Asokan, Xuejun Chen, Chen-Hsiang Shen, Gwo-Yu Chuang, Eun Sung Yang, Huiyi Miao, Yuge Wang, Anthony S. Fauci, Peter D. Kwong, John R. Mascola, and Paolo Lusso

Subjects

Science

Abstract

Quaternary contacts mediated by an extended heavy-chain framework region 3 (FR3) have been shown to improve binding to HIV envelope and virus neutralization for a few antibodies. Here, Liu et al. engraft such an FR3 loop onto several potent broadly neutralizing antibodies, resulting in improved neutralization activity and pharmacokinetics.

Published

2019

13. Sequence-Signature Optimization Enables Improved Identification of Human HV6-1-Derived Class Antibodies That Neutralize Diverse Influenza A Viruses

Author

Gwo-Yu Chuang, Chen-Hsiang Shen, Crystal Sao-Fong Cheung, Jason Gorman, Adrian Creanga, M. Gordon Joyce, Kwanyee Leung, Reda Rawi, Lingshu Wang, Eun Sung Yang, Yongping Yang, Baoshan Zhang, Yi Zhang, Masaru Kanekiyo, Tongqing Zhou, Brandon J. DeKosky, Barney S. Graham, John R. Mascola, and Peter D. Kwong

Subjects

antibody identification, hemagglutinin stem, influenza, iterative optimization, multidonor class antibody, neutralizing antibody, Immunologic diseases. Allergy, RC581-607

Abstract

Sequence signatures of multidonor broadly neutralizing influenza antibodies can be used to quantify the prevalence of B cells with virus-neutralizing potential to accelerate development of broadly protective vaccine strategies. Antibodies of the same class share similar recognition modes and developmental pathways, and several antibody classes have been identified that neutralize diverse group 1- and group 2-influenza A viruses and have been observed in multiple human donors. One such multidonor antibody class, the HV6-1-derived class, targets the stem region of hemagglutinin with extraordinary neutralization breadth. Here, we use an iterative process to combine informatics, biochemical, and structural analyses to delineate an improved sequence signature for HV6-1-class antibodies. Based on sequence and structure analyses of known HV6-1 class antibodies, we derived a more inclusive signature (version 1), which we used to search for matching B-cell transcripts from published next-generation sequencing datasets of influenza vaccination studies. We expressed selected antibodies, evaluated their function, and identified amino acid-level requirements from which to refine the sequence signature (version 2). The cryo-electron microscopy structure for one of the signature-identified antibodies in complex with hemagglutinin confirmed motif recognition to be similar to known HV6-1-class members, MEDI8852 and 56.a.09, despite differences in recognition-loop length. Threading indicated the refined signature to have increased accuracy, and signature-identified heavy chains, when paired with the light chain of MEDI8852, showed neutralization comparable to the most potent members of the class. Incorporating sequences of additional class members thus enables an improved sequence signature for HV6-1-class antibodies, which can identify class members with increased accuracy.

Published

2021

14. Glycan Positioning Impacts HIV-1 Env Glycan-Shield Density, Function, and Recognition by Antibodies

Author

Qing Wei, Audra A. Hargett, Barbora Knoppova, Alexandra Duverger, Reda Rawi, Chen-Hsiang Shen, S. Katie Farney, Stacy Hall, Rhubell Brown, Brandon F. Keele, Sonya L. Heath, Michael S. Saag, Olaf Kutsch, Gwo-Yu Chuang, Peter D. Kwong, Zina Moldoveanu, Milan Raska, Matthew B. Renfrow, and Jan Novak

Subjects

Biological Sciences, Biochemistry, Glycobiology, Microbiology, Virology, Science

Abstract

Summary: HIV-1 envelope (Env) N-glycosylation impact virus-cell entry and immune evasion. How each glycan interacts to shape the Env-protein-sugar complex and affects Env function is not well understood. Here, analysis of two Env variants from the same donor, with differing functional characteristics and N-glycosylation-site composition, revealed that changes to key N-glycosylation sites affected the Env structure at distant locations and had a ripple effect on Env-wide glycan processing, virus infectivity, antibody recognition, and virus neutralization. Specifically, the N262 glycan, although not in the CD4-binding site, modulated Env binding to the CD4 receptor, affected Env recognition by several glycan-dependent neutralizing antibodies, and altered site-specific glycosylation heterogeneity, with, for example, N448 displaying limited glycan processing. Molecular-dynamic simulations visualized differences in glycan density and how specific oligosaccharide positions can move to compensate for a glycan loss. This study demonstrates how changes in individual glycans can alter molecular dynamics, processing, and function of the Env-glycan shield.

Published

2020

15. Distinct disease features in chimpanzees infected with a precore HBV mutant associated with acute liver failure in humans.

Author

Zhaochun Chen, Ronald E Engle, Chen-Hsiang Shen, Huaying Zhao, Peter W Schuck, Emily J Danoff, Hanh Nguyen, Norihisa Nishimura, Kevin W Bock, Ian N Moore, Peter D Kwong, Robert H Purcell, Sugantha Govindarajan, and Patrizia Farci

Subjects

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

Abstract

Transmission to chimpanzees of a precore hepatitis B virus (HBV) mutant implicated in acute liver failure (ALF) in humans did not cause ALF nor the classic form of acute hepatitis B (AHB) seen upon infection with the wild-type HBV strain, but rather a severe AHB with distinct disease features. Here, we investigated the viral and host immunity factors responsible for the unusual severity of AHB associated with the precore HBV mutant in chimpanzees. Archived serial serum and liver specimens from two chimpanzees inoculated with a precore HBV mutant implicated in ALF and two chimpanzees inoculated with wild-type HBV were studied. We used phage-display library and next-generation sequencing (NGS) technologies to characterize the liver antibody response. The results obtained in severe AHB were compared with those in classic AHB and HBV-associated ALF in humans. Severe AHB was characterized by: (i) the highest alanine aminotransferase (ALT) peaks ever seen in HBV transmission studies with a significantly shorter incubation period, compared to classic AHB; (ii) earlier HBsAg clearance and anti-HBs seroconversion with transient or undetectable hepatitis B e antigen (HBeAg); (iii) limited inflammatory reaction relative to hepatocellular damage at the ALT peak with B-cell infiltration, albeit less extensive than in ALF; (iv) detection of intrahepatic germline antibodies against hepatitis B core antigen (HBcAg) by phage-display libraries in the earliest disease phase, as seen in ALF; (v) lack of intrahepatic IgM anti-HBcAg Fab, as seen in classic AHB, but at variance with ALF; and (vi) higher proportion of antibodies in germline configuration detected by NGS in the intrahepatic antibody repertoire compared to classic AHB, but lower than in ALF. This study identifies distinct outcome-specific features associated with severe AHB caused by a precore HBV mutant in chimpanzees, which bear closer resemblance to HBV ALF than to classic AHB. Our data suggest that precore HBV mutants carry an inherently higher pathogenicity that, in addition to specific host factors, may play a critical role in determining the severity of acute HBV disease.

Published

2020

16. Structure of Super-Potent Antibody CAP256-VRC26.25 in Complex with HIV-1 Envelope Reveals a Combined Mode of Trimer-Apex Recognition

Author

Jason Gorman, Gwo-Yu Chuang, Yen-Ting Lai, Chen-Hsiang Shen, Jeffrey C. Boyington, Aliaksandr Druz, Hui Geng, Mark K. Louder, Krisha McKee, Reda Rawi, Raffaello Verardi, Yongping Yang, Baoshan Zhang, Nicole A. Doria-Rose, Bob Lin, Penny L. Moore, Lynn Morris, Lawrence Shapiro, John R. Mascola, and Peter D. Kwong

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Antibodies targeting the V1V2 apex of the HIV-1 envelope (Env) trimer comprise one of the most commonly elicited categories of broadly neutralizing antibodies. Structures of these antibodies indicate diverse modes of Env recognition typified by antibodies of the PG9 class and the PGT145 class. The mode of recognition, however, has been unclear for the most potent of the V1V2 apex-targeting antibodies, CAP256-VRC26.25 (named for donor-lineage.clone and referred to hereafter as VRC26.25). Here, we determine the cryoelectron microscopy structure at 3.7 Å resolution of the antigen-binding fragment of VRC26.25 in complex with the Env trimer thought to have initiated the lineage. The 36-residue protruding loop of VRC26.25 displays recognition incorporating both strand-C interactions similar to the PG9 class and V1V2 apex insertion similar to the PGT145 class. Structural elements of separate antibody classes can thus intermingle to form a “combined” class, which in this case yields an antibody of extraordinary potency. : Antibody CAP256-VRC26.25 is one of the most potent known HIV-1-neutralizing antibodies. Gorman et al. determine the cryo-EM structure of this antibody in complex with the Env trimer that initiated the antibody lineage. The structure reveals how elements of distinct antibody classes can intermingle to yield an antibody of extraordinary potency. Keywords: broadly neutralizing antibody, HIV-1 envelope trimer, multidonor antibody class, PCT64, PG9, PGDM1400, PGT145, tyrosine sulfation, V1V2 apex recognition

Published

2020

17. Quantification of the Impact of the HIV-1-Glycan Shield on Antibody Elicitation

Author

Tongqing Zhou, Nicole A. Doria-Rose, Cheng Cheng, Guillaume B.E. Stewart-Jones, Gwo-Yu Chuang, Michael Chambers, Aliaksandr Druz, Hui Geng, Krisha McKee, Young Do Kwon, Sijy O’Dell, Mallika Sastry, Stephen D. Schmidt, Kai Xu, Lei Chen, Rita E. Chen, Mark K. Louder, Marie Pancera, Timothy G. Wanninger, Baoshan Zhang, Anqi Zheng, S. Katie Farney, Kathryn E. Foulds, Ivelin S. Georgiev, M. Gordon Joyce, Thomas Lemmin, Sandeep Narpala, Reda Rawi, Cinque Soto, John-Paul Todd, Chen-Hsiang Shen, Yaroslav Tsybovsky, Yongping Yang, Peng Zhao, Barton F. Haynes, Leonidas Stamatatos, Michael Tiemeyer, Lance Wells, Diana G. Scorpio, Lawrence Shapiro, Adrian B. McDermott, John R. Mascola, and Peter D. Kwong

Subjects

CD4-binding site, crystal structure, envelope glycoprotein, glycan shield, glycomics, HIV-1, immunogen design, immunogenicity, targeted deglycosylation, vaccine design, Biology (General), QH301-705.5

Abstract

While the HIV-1-glycan shield is known to shelter Env from the humoral immune response, its quantitative impact on antibody elicitation has been unclear. Here, we use targeted deglycosylation to measure the impact of the glycan shield on elicitation of antibodies against the CD4 supersite. We engineered diverse Env trimers with select glycans removed proximal to the CD4 supersite, characterized their structures and glycosylation, and immunized guinea pigs and rhesus macaques. Immunizations yielded little neutralization against wild-type viruses but potent CD4-supersite neutralization (titers 1: >1,000,000 against four-glycan-deleted autologous viruses with over 90% breadth against four-glycan-deleted heterologous strains exhibiting tier 2 neutralization character). To a first approximation, the immunogenicity of the glycan-shielded protein surface was negligible, with Env-elicited neutralization (ID50) proportional to the exponential of the protein-surface area accessible to antibody. Based on these high titers and exponential relationship, we propose site-selective deglycosylated trimers as priming immunogens to increase the frequency of site-targeting antibodies.

Published

2017

18. Diverse Murine Vaccinations Reveal Distinct Antibody Classes to Target Fusion Peptide and Variation in Peptide Length to Improve HIV Neutralization

Author

Mallika Sastry, Anita Changela, Jason Gorman, Kai Xu, Gwo-Yu Chuang, Chen-Hsiang Shen, Cheng Cheng, Hui Geng, Sijy O'Dell, Li Ou, Reda Rawi, Mateo Reveiz, Guillaume B. E. Stewart-Jones, Shuishu Wang, Baoshan Zhang, Tongqing Zhou, Andrea Biju, Michael Chambers, Xuejun Chen, Angela R. Corrigan, Bob C. Lin, Mark K. Louder, Krisha McKee, Alexandra F. Nazzari, Adam S. Olia, Danealle K. Parchment, Edward K. Sarfo, Tyler Stephens, Jonathan Stuckey, Yaroslav Tsybovsky, Raffaello Verardi, Yiran Wang, Cheng-Yan Zheng, Yuling Chen, Nicole A. Doria-Rose, Adrian B. McDermott, John R. Mascola, and Peter D. Kwong

Subjects

Virology, Insect Science, Immunology, Microbiology

Abstract

The HIV-1 fusion peptide has been identified as a site for elicitation of broadly neutralizing antibodies, with prior studies demonstrating that priming with fusion peptide-based immunogens and boosting with soluble envelope (Env) trimers can elicit cross-clade HIV-1-neutralizing responses. To improve the neutralizing breadth and potency of fusion peptide-directed responses, we evaluated vaccine regimens that incorporated diverse fusion peptide-conjugates and Env trimers with variation in fusion peptide length and sequence.

Published

2023

19. Highly protective antimalarial antibodies via precision library generation and yeast display screening

Author

Bailey B. Banach, Prabhanshu Tripathi, Lais Da Silva Pereira, Jason Gorman, Thuy Duong Nguyen, Marlon Dillon, Ahmed S. Fahad, Patience K. Kiyuka, Bharat Madan, Jacy R. Wolfe, Brian Bonilla, Barbara Flynn, Joseph R. Francica, Nicholas K. Hurlburt, Neville K. Kisalu, Tracy Liu, Li Ou, Reda Rawi, Arne Schön, Chen-Hsiang Shen, I-Ting Teng, Baoshan Zhang, Marie Pancera, Azza H. Idris, Robert A. Seder, Peter D. Kwong, and Brandon J. DeKosky

Subjects

Antimalarials, Cryoelectron Microscopy, Malaria Vaccines, Plasmodium falciparum, Immunology, Protozoan Proteins, Antibodies, Protozoan, Humans, Immunology and Allergy, Saccharomyces cerevisiae

Abstract

The monoclonal antibody CIS43 targets the Plasmodium falciparum circumsporozoite protein (PfCSP) and prevents malaria infection in humans for up to 9 mo following a single intravenous administration. To enhance the potency and clinical utility of CIS43, we used iterative site-saturation mutagenesis and DNA shuffling to screen precise gene-variant yeast display libraries for improved PfCSP antigen recognition. We identified several mutations that improved recognition, predominately in framework regions, and combined these to produce a panel of antibody variants. The most improved antibody, CIS43_Var10, had three mutations and showed approximately sixfold enhanced protective potency in vivo compared to CIS43. Co-crystal and cryo-electron microscopy structures of CIS43_Var10 with the peptide epitope or with PfCSP, respectively, revealed functional roles for each of these mutations. The unbiased site-directed mutagenesis and screening pipeline described here represent a powerful approach to enhance protective potency and to enable broader clinical use of antimalarial antibodies.

Published

2022

20. Cryo-EM structures of anti-malarial antibody L9 with circumsporozoite protein reveal trimeric L9 association and complete 27-residue epitope

Author

Prabhanshu Tripathi, Michael F. Bender, Haotian Lei, Lais Da Silva Pereira, Chen-Hsiang Shen, Brian Bonilla, Marlon Dillon, Li Ou, Marie Pancera, Lawrence T. Wang, Baoshan Zhang, Facundo D. Batista, Azza H. Idris, Robert A. Seder, and Peter D. Kwong

Subjects

Structural Biology, Molecular Biology

Published

2023

21. Structure of an Influenza Group 2-Neutralizing Antibody Targeting the Hemagglutinin Stem Supersite

Author

Crystal Sao-Fong Cheung, Jason Gorman, Sarah F. Andrews, Reda Rawi, Mateo Reveiz, Chen-Hsiang Shen, Yiran Wang, Darcy R. Harris, Alexandra F. Nazzari, Adam S. Olia, Julie Raab, I-Ting Teng, Raffaello Verardi, Shuishu Wang, Yongping Yang, Gwo-Yu Chuang, Adrian B. McDermott, Tongqing Zhou, and Peter D. Kwong

Subjects

Hemagglutinins, Structural Biology, Influenza Vaccines, Influenza, Human, Humans, Hemagglutinin Glycoproteins, Influenza Virus, Influenza A Virus, H7N9 Subtype, Molecular Biology, Antibodies, Neutralizing, Article

Abstract

Several influenza antibodies with broad group 2 neutralization have recently been isolated. Here, we analyze the structure, class, and binding of one of these antibodies from an H7N9 vaccine trial, 315-19-1D12. The cryo-EM structure of 315-19-1D12 Fab in complex with the hemagglutinin (HA) trimer revealed the antibody to recognize the helix A region of the HA stem, at the supersite of vulnerability recognized by group 1-specific and by cross-group-neutralizing antibodies. 315-19-1D12 was derived from HV1-2 and KV2-28 genes and appeared to form a new antibody class. Bioinformatic analysis indicated its group 2 neutralization specificity to be a consequence of four key residue positions. We specifically tested the impact of the group 1-specific N33 glycan, which decreased but did not abolish group 2 binding of 315-19-1D12. Overall, this study highlights the recognition of a broad group 2-neutralizing antibody, revealing unexpected diversity in neutralization specificity for antibodies that recognize the HA stem supersite.

Published

2022

22. In Silico Improvement of Highly Protective Anti-Malarial Antibodies

Author

Mateo Reveiz, Prabhanshu Tripathi, Lais Da Silva Pereira, Patience Kiyuka, Tracy Liu, Baoshan Zhang, Yongping Yang, Brian G. Bonilla, Marlon Dillon, Myungjin Lee, Chen-Hsiang Shen, Arne Schön, Sven Kratochvil, Facundo D. Batista, Azza H. Idris, Robert A. Seder, Peter D. Kwong, and Reda Rawi

Abstract

SUMMARYAntibody CIS43 binds Plasmodium falciparum circumsporozoite protein (PfCSP) and protects against malaria, as recently demonstrated clinically. To improve the efficacy of CIS43, we developed an in silico pipeline to optimize the interaction energy of CIS43 to its junctional epitope (peptide 21: PfCSP residues 101-115). Starting from two improved CIS43 variants, recently elicited from a CIS43-germline knock-in mice, single and double amino acid substitutions in the peptide 21-proximal heavy (VH) and light (VL) variable regions were introduced. CIS43-variants, selected on the basis of improved in silico interface and stability energies, showed increased affinity to peptide 21 and superior malaria-protective efficacy. The best designed variant, antibody P3-43, was significantly more protective than its template antibody m43.151, with greater liver-burden protection than the current best-in-class (antibody iGL-CIS43.D3). Crystal structures of improved antibodies revealed atomic-level interactions explaining gains in binding affinity. The reported pipeline provides a powerful in silico approach to improve antibody functionality.

Published

2022

23. Next‐generation sequencing of the intrahepatic antibody repertoire delineates a unique B‐cell response in HBV‐associated acute liver failure

Author

Fausto Zamboni, Zhaochun Chen, Ronald E. Engle, Patrizia Farci, Peter D. Kwong, Robert H. Purcell, and Chen-Hsiang Shen

Subjects

Hepatitis B virus, Somatic hypermutation, Biology, medicine.disease_cause, Germline, 03 medical and health sciences, 0302 clinical medicine, Antibody Repertoire, Virology, medicine, Humans, Hepatitis Antibodies, 030212 general & internal medicine, B cell, B-Lymphocytes, Hepatology, digestive, oral, and skin physiology, High-Throughput Nucleotide Sequencing, Liver Failure, Acute, Hepatitis B, Immunoglobulin Class Switching, Isotype, Infectious Diseases, medicine.anatomical_structure, Immunoglobulin M, Immunoglobulin G, Humoral immunity, Immunology, biology.protein, 030211 gastroenterology & hepatology, Antibody

Abstract

Hepatitis B virus (HBV) is a major cause of acute liver failure (ALF) worldwide. While liver damage in classic acute hepatitis B is believed to be T-cell mediated, the pathogenesis of HBV-associated ALF remains largely unknown. Access to liver specimens from well-characterized patients with HBV-associated ALF provided us with the opportunity to perform next-generation sequencing (NGS) of the entire VH repertoires of IgM and IgG from the livers of four ALF patients, a control liver donor and a patient with chronic HBV infection. We found that ALF is not associated with expansion of specific B-cell lineages. However, NGS showed that the intrahepatic VH repertoires from ALF patients were characterized by the abundant presence of antibodies in germline configuration in contrast to their marginal prevalence in controls. Moreover, NGS identified a large number of VH genes in germline configuration with identical VDJ sequences in the IgM and IgG repertoires in all four ALF patients, indicating that isotype switch from IgM to IgG had occurred without somatic hypermutation. The results of this study indicate that the presence of intrahepatic antibodies in unmutated germline configuration is a broad phenomenon in the global antibody repertoire generated from total RNA derived from whole-liver tissue that is strongly associated with ALF, suggesting a major role of T cell-independent humoral immunity in the pathogenesis of ALF.

Published

2020

24. Vaccine-elicited murine antibody WS6 neutralizes diverse beta-coronaviruses by recognizing a helical stem supersite of vulnerability

Author

Wei Shi, Lingshu Wang, Tongqing Zhou, Mallika Sastry, Eun Sung Yang, Yi Zhang, Man Chen, Xuejun Chen, Misook Choe, Adrian Creanga, Kwan Leung, Adam S. Olia, Amarendra Pegu, Reda Rawi, Arne Schön, Chen-Hsiang Shen, Erik-Stephane D. Stancofski, Chloe Adrienna Talana, I-Ting Teng, Shuishu Wang, Kizzmekia S. Corbett, Yaroslav Tsybovsky, John R. Mascola, and Peter D. Kwong

Subjects

Vaccines, crystal structure, SARS-CoV-2, viruses, virus diseases, COVID-19, beta-coronavirus, biochemical phenomena, metabolism, and nutrition, respiratory system, Antibodies, Viral, Antibodies, Neutralizing, Article, respiratory tract diseases, broadly neutralizing antibody, Mice, Structural Biology, Spike Glycoprotein, Coronavirus, vaccine design, Animals, S2-directed antibody, Molecular Biology

Abstract

SummaryImmunization with SARS-CoV-2 spike elicits diverse antibodies, but can any of these neutralize broadly? Here, we report the isolation and characterization of antibody WS6, from a mouse immunized with mRNA encoding the SARS-CoV-2 spike. WS6 bound diverse beta-coronavirus spikes and neutralized SARS-CoV-2 variants, SARS-CoV, and related sarbecoviruses. Epitope mapping revealed WS6 to target a region in the S2 subunit, which was conserved among SARS-CoV-2, MERS-CoV, and hCoV-OC43. The crystal structure at 2-Å resolution of WS6 with its S2 epitope revealed recognition to center on a conserved helix, which was occluded in both prefusion and post-fusion spike conformations. Structural and neutralization analyses indicated WS6 to neutralize by inhibiting fusion, post-viral attachment. Comparison of WS6 to other antibodies recently identified from convalescent donors or mice immunized with diverse spikes indicated a stem-helical supersite – centered on hydrophobic residues Phe1148, Leu1152, Tyr1155, and Phe1156 – to be a promising target for vaccine design.HighlightsSARS-CoV-2 spike mRNA-immunized mouse elicited an antibody, WS6, that cross reacts with spikes of diverse human and bat beta-coronavirusesWS6 neutralizes SARS-CoV-2 variants, SARS-CoV, and related virusesCrystal structure at 2-Å resolution of WS6 in complex with a conserved S2 peptide reveals recognition of a helical epitopeWS6 neutralizes by inhibition of fusion, post-viral attachmentWS6 recognizes a supersite of vulnerability also recognized by other recently identified antibodiesHelical supersite of vulnerability comprises a hydrophobic cluster spanning three helical turns, with acid residues framing the center turnGenetic and structural analysis indicate supersite recognition to be compatible with diverse antibody ontogenies

Published

2022

25. Interprotomer disulfide-stabilized variants of the human metapneumovirus fusion glycoprotein induce high titer-neutralizing responses

Author

John-Paul Todd, Antonio Lanzavecchia, Wing-Pui Kong, Yaroslav Tsybovsky, Gwo-Yu Chuang, John R. Mascola, Peter L. Collins, Lijuan Yang, Jason Gorman, M. Gordon Joyce, Davide Corti, Mallika Sastry, Raffaello Verardi, Diana G. Scorpio, Guillaume Stewart-Jones, Yongping Yang, Ursula J. Buchholz, Cheng Cheng, Kathryn E. Foulds, Adam S. Olia, Chen-Hsiang Shen, Baoshan Zhang, Li Ou, and Peter D. Kwong

Subjects

Antigenicity, viruses, Trimer, Antibodies, Viral, Epitope, Neutralization, Epitopes, Mice, Human metapneumovirus, Animals, Humans, Disulfides, Promoter Regions, Genetic, Glycoproteins, chemistry.chemical_classification, Multidisciplinary, biology, Chemistry, Immunogenicity, virus diseases, Biological Sciences, biology.organism_classification, Virology, Antibodies, Neutralizing, respiratory tract diseases, Titer, Mutation, Macaca, Immunization, Metapneumovirus, Glycoprotein

Abstract

Human metapneumovirus (HMPV) is a major cause of respiratory disease worldwide, particularly among children and the elderly. Although there is no licensed HMPV vaccine, promising candidates have been identified for related pneumoviruses based on the structure-based stabilization of the fusion (F) glycoprotein trimer, with prefusion-stabilized F glycoprotein trimers eliciting significantly higher neutralizing responses than their postfusion F counterparts. However, immunization with HMPV F trimers in either prefusion or postfusion conformations has been reported to elicit equivalent neutralization responses. Here we investigate the impact of stabilizing disulfides, especially interprotomer disulfides (IP-DSs) linking protomers of the F trimer, on the elicitation of HMPV-neutralizing responses. We designed F trimer disulfides, screened for their expression, and used electron microscopy (EM) to confirm their formation, including that of an unexpected postfusion variant. In mice, IP-DS–stabilized prefusion and postfusion HMPV F elicited significantly higher neutralizing responses than non–IP-DS–stabilized HMPV Fs. In macaques, the impact of IP-DS stabilization was more measured, although IP-DS–stabilized variants of either prefusion or postfusion HMPV F induced neutralizing responses many times the average titers observed in a healthy human cohort. Serological and absorption-based analyses of macaque responses revealed elicited HMPV-neutralizing responses to be absorbed differently by IP-DS–containing and by non–IP-DS–containing postfusion Fs, suggesting IP-DS stabilization to alter not only the immunogenicity of select epitopes but their antigenicity as well. We speculate the observed increase in immunogenicity by IP-DS trimers to be related to reduced interprotomer flexibility within the HMPV F trimer.

Published

2021

26. Structural basis of LAIR1 targeting by polymorphic Plasmodium RIFINs

Author

Peter D. Kwong, Shuishu Wang, Raffaello Verardi, Jason Gorman, Chen-Hsiang Shen, Gwo-Yu Chuang, Kai Xu, Baoshan Zhang, Yongping Yang, Yiran Wang, Tyler Stephens, Kevin Liu, Yaroslav Tsybovsky, S. Katie Farney, Tongqing Zhou, Antonio Lanzavecchia, Luca Piccoli, and Yiwei Chen

Subjects

Sequence analysis, Science, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, General Physics and Astronomy, Antigens, Protozoan, Crystallography, X-Ray, medicine.disease_cause, Plasmodium, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Protein Domains, Antigen, parasitic diseases, medicine, Humans, Malaria, Falciparum, Receptors, Immunologic, Receptor, X-ray crystallography, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, Multidisciplinary, biology, LAIR1, Membrane Proteins, General Chemistry, biology.organism_classification, Antigenic Variation, Malaria, biology.protein, Antibody, 030217 neurology & neurosurgery

Abstract

RIFIN, a large family of Plasmodium variant surface antigens, plays a crucial role in malaria pathogenesis by mediating immune suppression through activation of inhibitory receptors such as LAIR1, and antibodies with LAIR1 inserts have been identified that bind infected erythrocytes through RIFIN. However, details of RIFIN-mediated LAIR1 recognition and receptor activation have been unclear. Here, we use negative-stain EM to define the architecture of LAIR1-inserted antibodies and determine crystal structures of RIFIN-variable 2 (V2) domain in complex with a LAIR1 domain. These structures reveal the LAIR1-binding region of RIFIN to be hydrophobic and membrane-distal, to exhibit extensive structural diversity, and to interact with RIFIN-V2 in a one-to-one fashion. Through structural and sequence analysis of various LAIR1 constructs, we identify essential elements of RIFIN-binding on LAIR1. Furthermore, a structure-derived LAIR1-binding sequence signature ascertained >20 LAIR1-binding RIFINs, including some from P. falciparum field strains and Plasmodium species infecting gorillas and chimpanzees., Nature Communications, 12, ISSN:2041-1723

Published

2021

27. Improvement of antibody functionality by structure-guided paratope engraftment

Author

Mangaiarkarasi Asokan, Anthony S. Fauci, Peter D. Kwong, Huiyi Miao, Paolo Lusso, Peng Zhang, Gwo-Yu Chuang, Xuejun Chen, Eun Sung Yang, Yuge Wang, John R. Mascola, Qingbo Liu, Amarendra Pegu, Chen-Hsiang Shen, Mark K. Louder, Yen-Ting Lai, and Reda Rawi

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, Science, Immunoglobulin Variable Region, General Physics and Astronomy, Mutagenesis (molecular biology technique), HIV Infections, Mice, Transgenic, 02 engineering and technology, Protomer, HIV Antibodies, HIV Envelope Protein gp120, General Biochemistry, Genetics and Molecular Biology, Epitope, Article, 03 medical and health sciences, Epitopes, Mice, Animals, Humans, Binding site, Framework region, lcsh:Science, Multidisciplinary, biology, Chemistry, General Chemistry, 021001 nanoscience & nanotechnology, Virology, Antibodies, Neutralizing, Macaca mulatta, Disease Models, Animal, 030104 developmental biology, Epitope mapping, HEK293 Cells, biology.protein, HIV-1, Mutagenesis, Site-Directed, Paratope, Female, lcsh:Q, Binding Sites, Antibody, Antibody, 0210 nano-technology, Epitope Mapping

Abstract

Broadly neutralizing antibodies (bNAbs) represent a promising alternative to antiretroviral drugs for HIV-1 prevention and treatment. Selected antibodies to the CD4-binding site bolster envelope trimer binding via quaternary contacts. Here, we rationally engraft a new paratope, i.e., the extended heavy-chain framework region 3 (FR3) loop of VRC03, which mediates quaternary interaction, onto several potent bNAbs, enabling them to reach an adjacent gp120 protomer. The interactive quaternary surface is delineated by solving the crystal structure of two FR3 loop-chimeric antibodies. Chimerization enhances the neutralizing activity of several potent bNAbs against a majority of global HIV-1 strains. Compared to unmodified antibodies, chimeric antibodies display lower autoreactivity and prolonged in vivo half-life in huFcRn mice and rhesus macaques. Thus, paratope engraftment may be used to expand the epitope repertory of natural antibodies, improving their functionality for disease prevention and treatment., Quaternary contacts mediated by an extended heavy-chain framework region 3 (FR3) have been shown to improve binding to HIV envelope and virus neutralization for a few antibodies. Here, Liu et al. engraft such an FR3 loop onto several potent broadly neutralizing antibodies, resulting in improved neutralization activity and pharmacokinetics.

Published

2019

28. A single residue in influenza virus H2 hemagglutinin enhances the breadth of the B cell response elicited by H2 vaccination

Author

Sarah F. Andrews, Julie E. Raab, Jason Gorman, Rebecca A. Gillespie, Crystal S. F. Cheung, Reda Rawi, Lauren Y. Cominsky, Jeffrey C. Boyington, Adrian Creanga, Chen-Hsiang Shen, Darcy R. Harris, Adam S. Olia, Alexandra F. Nazzari, Tongqing Zhou, Katherine V. Houser, Grace L. Chen, John R. Mascola, Barney S. Graham, Masaru Kanekiyo, Julie E. Ledgerwood, Peter D. Kwong, and Adrian B. McDermott

Subjects

Clinical Trials, Phase I as Topic, Influenza A Virus, H5N1 Subtype, Vaccination, Hemagglutinin Glycoproteins, Influenza Virus, General Medicine, Antibodies, Viral, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology, Epitopes, Hemagglutinins, Influenza Vaccines, Influenza, Human, Humans, Child

Abstract

Conserved epitopes on the influenza hemagglutinin (HA) stem are an attractive target for universal vaccine strategies as they elicit broadly neutralizing antibodies. Such antibody responses to stem-specific epitopes have been extensively characterized for HA subtypes H1 and H5 in humans. H2N2 influenza virus circulated 50 years ago and represents a pandemic threat due to the lack of widespread immunity, but, unlike H1 and H5, the H2 HA stem contains Phe45

Published

2021

29. Vaccination in a humanized mouse model elicits highly protective PfCSP-targeting anti-malarial antibodies

Author

Joseph R. Francica, Eleonora Melzi, Baoshan Zhang, Kai Xu, Ying-Cing Lin, Kareen Seignon, Tracy Liu, Chen-Hsiang Shen, Gwo-Yu Chuang, John Warner, Marie Pancera, Usha Nair, Arne Schön, Lais Pereira, Prabhanshu Tripathi, Michael T. Waring, Peter D. Kwong, Sven Kratochvil, Reda Rawi, Lawrence T. Wang, Marlon Dillon, Li Ou, Yongping Yang, Barbara J. Flynn, Azza H. Idris, Robert A. Seder, Kathrin H Kirsch, Neville K. Kisalu, Brian Bonilla, Patience K. Kiyuka, Mateo Reveiz, Facundo D. Batista, and Johan Arnold

Subjects

Immunology, B-cell receptor, Plasmodium falciparum, B-Lymphocyte Subsets, Protozoan Proteins, Antibodies, Protozoan, Mice, SCID, Article, Antibodies, Epitope, Epitopes, Mice, Structure-Activity Relationship, Immune system, Immunogenicity, Vaccine, Antigen, Malaria Vaccines, Vaccines, DNA, Immunology and Allergy, Animals, Humans, Immune Evasion, biology, Vaccination, Germinal center, Virology, Adoptive Transfer, Malaria, Circumsporozoite protein, Disease Models, Animal, Infectious Diseases, Humanized mouse, biology.protein, Antibody, Genetic Engineering

Abstract

Repeat antigens, such as the Plasmodium falciparum circumsporozoite protein (PfCSP), use both sequence degeneracy and structural diversity to evade the immune response. A few PfCSP-directed antibodies have been identified that are effective at preventing malaria infection, including CIS43, but how these repeat-targeting antibodies might be improved has been unclear. Here, we engineered a humanized mouse model in which B cells expressed inferred human germline CIS43 (iGL-CIS43) B cell receptors and used both vaccination and bioinformatic analysis to obtain variant CIS43 antibodies with improved protective capacity. One such antibody, iGL-CIS43.D3, was significantly more potent than the current best-in-class PfCSP-directed antibody. We found that vaccination with a junctional epitope peptide was more effective than full-length PfCSP at recruiting iGL-CIS43 B cells to germinal centers. Structure-function analysis revealed multiple somatic hypermutations that combinatorically improved protection. This mouse model can thus be used to understand vaccine immunogens and to develop highly potent anti-malarial antibodies.

Published

2021

30. Automated Design by Structure-Based Stabilization and Consensus Repair to Achieve Prefusion-Closed Envelope Trimers in a Wide Variety of HIV Strains

Author

Raffaello Verardi, Reda Rawi, Gwo-Yu Chuang, Lucy Rutten, Yongping Yang, Tongqing Zhou, Peter D. Kwong, Johannes P. M. Langedijk, Jarek Juraszek, Yaroslav Tsybovsky, Chen-Hsiang Shen, Baoshan Zhang, Yen-Ting Lai, Sven Blokland, and Adam S. Olia

Subjects

0301 basic medicine, Consensus, Chemistry, Hiv 1 vaccine, Protein design, Human immunodeficiency virus (HIV), env Gene Products, Human Immunodeficiency Virus, virus diseases, Antigenic analysis, Trimer, Computational biology, HIV Antibodies, medicine.disease_cause, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine, HIV-1, Structure based, Humans, Protein Multimerization, 030217 neurology & neurosurgery

Abstract

Summary Soluble envelope (Env) trimers, stabilized in a prefusion-closed conformation, can elicit neutralizing responses against HIV-1 strains closely related to the immunizing trimer. However, to date such stabilization has succeeded with only a limited number of HIV-1 strains. To address this issue, here we develop ADROITrimer, an automated procedure involving structure-based stabilization and consensus repair, and generate “RnS-DS-SOSIP”-stabilized Envs from 180 diverse Env sequences. The vast majority of these RnS-DS-SOSIP Envs fold into prefusion-closed conformations as judged by antigenic analysis and size exclusion chromatography. Additionally, representative strains from clades AE, B, and C are stabilized in prefusion-closed conformations as shown by negative-stain electron microscopy, and the crystal structure of a clade A strain MI369.A5 Env trimer provides 3.5 A resolution detail into stabilization and repair mutations. The automated procedure reported herein that yields well-behaved, soluble, prefusion-closed Env trimers from a majority of HIV-1 strains could have substantial impact on the development of an HIV-1 vaccine.

Published

2020

31. Impact of Glycan Positioning on HIV-1 Env Glycan Shield Density, Function, and Antibody Recognition

Author

Stacy Hall, Olaf Kutsch, Sonya L. Heath, Jan Novak, Rhubell Brown, Matthew B. Renfrow, Barbora Knoppova, Michael S. Saag, Audra A. Harget, S. Katie Farney, Zina Moldoveanu, Gwo-Yu Chuang, Alexandra Duverger, Chen-Hsiang Shen, Milan Raska, Brandon F. Keele, Reda Ravi, Peter D. Kwong, and Qing Wei

Subjects

Infectivity, chemistry.chemical_classification, Glycan, Glycosylation, biology, viruses, virus diseases, Virus, Cell biology, carbohydrates (lipids), Glycomics, chemistry.chemical_compound, chemistry, biology.protein, Antibody, Receptor, Glycoprotein, Function (biology)

Abstract

N-glycans, which represent >50% mass of the HIV-1 envelope (Env) trimer, play important roles for virus-cell entry and immune evasion. How each glycan unit interacts to shape the Env protein-sugar complex and affects Env function is not well understood. Here, high-resolution glycomics analysis of two Env variants from the same donor, with differing functional characteristics and N-glycosylation-site composition, revealed that changes to key N-glycosylation-site not only affected the Env structure at distant locations, but also had a ripple effect on Env-wide glycan processing, virus infectivity, and antibody recognition and virus neutralization. Specifically, the N262 glycan, although not located in the CD4-binding site, controlled Env binding to the CD4 receptor, affected the recognition of Env by several glycan-dependent broadly neutralizing antibodies, and altered heterogeneity of glycosylation at several sites, with N156, N160, and N448 displaying limited glycan processing. Molecular dynamic simulations visualized how specific oligosaccharide positions can move to compensate for loss of a glycan. This study demonstrates how changes in individual glycan units can alter molecular dynamics and processing of the Env-glycan shield and, consequently, Env function.

Published

2020

32. Vaccination Induces Maturation of Diverse Unmutated VRC01-Class Precursors to HIV-1 Broadly Neutralizing Antibodies in an Ig-Humanized Mouse Model

Author

Xuejun Chen, Tongqing Zhou, Stephen D. Schmidt, Hongying Duan, Cheng Cheng, Gwo-Yu Chuang, Ying Gu, Mark K. Louder, Bob Lin, Chen-Hsiang Shen, Zizhang Sheng, Michelle X. Zheng, M. Gordon Joyce, Nicole Doria-Rose, Lawrence Shapiro, Ming Tian, Frederick W. Alt, Peter D. Kwong, and John Mascola

Published

2020

33. Molecular Dissection Of Human Antibody Responses Following Prefusion-Stabilized RSV F Vaccination

Author

Scott A. Rush, Pamela Costner, John R. Mascola, Morgan S.A. Gilman, Yi Zhang, Samuel Darko, Barney S. Graham, Chaim A. Schramm, Alexandrine Derrien-Colemyn, John Misasi, Guillaume Stewart-Jones, Bharat Madan, Peter D. Kwong, Martin R. Gaudinski, Chen-Hsiang Shen, Grace L. Chen, Kaitlyn M. Morabito, Amy Ransier, Jason S. McLellan, Michelle C. Crank, Larissa Ault, Tracy J. Ruckwardt, LaSonji A. Holman, Daniel C. Douek, Sarah A.M. Lucas, Emily Phung, Nina M. Berkowitz, Brandon J. DeKosky, Nicole A. Doria-Rose, Nancy J. Sullivan, Daniel Wrapp, Maryam Mukhamedova, Lingshu Wang, Lauren A. Chang, and Somia P. Hickman

Subjects

chemistry.chemical_classification, biology, Protein subunit, medicine.disease_cause, Virology, Vaccination, Respiratory syncytial virus (RSV), Polyclonal B cell response, Antigen, chemistry, Antibody Repertoire, medicine, biology.protein, Antibody, Glycoprotein

Abstract

An effective vaccine for RSV is an unrealized public health goal. Recently, a single dose of the prefusion-stabilized fusion (F) glycoprotein subunit vaccine (DS-Cav1) was shown to substantially increase serum neutralizing activity in healthy adults. To understand the induced B-cell repertoire at the single-cell level, we evaluated RSV F-specific B-cell responses before and after vaccination in six participants and identified 555 clonal lineages. DS-Cav1-induced lineages recognized the prefusion conformation of F (pre-F) and were genetically diverse. Expressed antibodies recognized all six previously defined antigenic sites on the pre-F trimer. Among the six vaccinees, we identified 34 public clonotypes. Structural analysis of two antibodies from a predominant clonotype revealed a common mode of recognition. Collectively, these findings demonstrate that vaccination with DS-Cav1 generates a diverse polyclonal response targeting all known antigenic sites present on pre-F.

Published

2020

34. Paired Heavy and Light Chain Signatures Contribute to Potent SARS-CoV-2 Neutralization in Public Antibody Responses

Author

Irene M. Francino Urdániz, Timothy A. Whitehead, Ahmed S. Fahad, Bailey B. Banach, Adam S. Olia, Phinikoula S. Katsamba, Sheila N. Lopez Acevedo, Lihong Liu, Manoj S. Nair, Alexandra Nazzari, Yaoxing Huang, Jacy R. Wolfe, Amy D. Laflin, Bharat Madan, Xiaoli Pan, Matheus Oliveira de Souza, Jude Bimela, David D. Ho, Pengfei Wang, Kwok-Yung Yuen, I-Ting Teng, Jian Yu, Yaroslav Tsybovsky, Eswar R. Reddem, Rajani Nimrania, Lawrence Shapiro, Brandon J. DeKosky, Gabriele Cerutti, Peter D. Kwong, Paul J. Steiner, Matias Gutiérrez-González, Yang Luo, Chen-Hsiang Shen, and Tongqing Zhou

Subjects

Antibody response, Coronavirus disease 2019 (COVID-19), biology, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), biology.protein, Yeast display, Antibody, Immunoglobulin light chain, Virology, Gene, Neutralization, Sequence (medicine)

Abstract

SummaryUnderstanding protective mechanisms of antibody recognition can inform vaccine and therapeutic strategies against SARS-CoV-2. We discovered a new antibody, 910-30, that targets the SARS-CoV-2 ACE2 receptor binding site as a member of a public antibody response encoded by IGHV3-53/IGHV3-66 genes. We performed sequence and structural analyses to explore how antibody features correlate with SARS-CoV-2 neutralization. Cryo-EM structures of 910-30 bound to the SARS-CoV-2 spike trimer revealed its binding interactions and ability to disassemble spike. Despite heavy chain sequence similarity, biophysical analyses of IGHV3-53/3-66 antibodies highlighted the importance of native heavy:light pairings for ACE2 binding competition and for SARS-CoV-2 neutralization. We defined paired heavy:light sequence signatures and determined antibody precursor prevalence to be ~1 in 44,000 human B cells, consistent with public antibody identification in several convalescent COVID-19 patients. These data reveal key structural and functional neutralization features in the IGHV3-53/3-66 public antibody class to accelerate antibody-based medical interventions against SARS-CoV-2.HighlightsA molecular study of IGHV3-53/3-66 public antibody responses reveals critical heavy and light chain features for potent neutralizationCryo-EM analyses detail the structure of a novel public antibody class member, antibody 910-30, in complex with SARS-CoV-2 spike trimerCryo-EM data reveal that 910-30 can both bind assembled trimer and can disassemble the SARS-CoV-2 spikeSequence-structure-function signatures defined for IGHV3-53/3-66 class antibodies including both heavy and light chainsIGHV3-53/3-66 class precursors have a prevalence of 1:44,000 B cells in healthy human antibody repertoires

Published

2020

35. Structural basis of glycan276-dependent recognition by HIV-1 broadly neutralizing antibodies

Author

Megan Kopp, Nicole A. Doria-Rose, Shuishu Wang, Gwo-Yu Chuang, Reda Rawi, Justin Taft, Chen-Hsiang Shen, Adam S. Olia, Mark K. Louder, Lawrence Shapiro, John R. Mascola, Baoshan Zhang, Christopher A. Cottrell, Jonathan L. Torres, Barton F. Haynes, Katarzyna Janowska, Rui Kong, Bob C. Lin, Kartik Manne, Peter D. Kwong, Priyamvada Acharya, Robert J. Edwards, Nelson R. Wu, Andrew B. Ward, Myron S. Cohen, Rory Henderson, and Tongqing Zhou

Subjects

Models, Molecular, Glycan, QH301-705.5, Protein Conformation, Human immunodeficiency virus (HIV), Priming (immunology), Trimer, glycan276, medicine.disease_cause, CD4 binding site, General Biochemistry, Genetics and Molecular Biology, antibody-antigen binding, Epitopes, Structure-Activity Relationship, Antibody Specificity, Polysaccharides, medicine, Humans, Biology (General), AIDS Vaccines, biology, Chemistry, Cryoelectron Microscopy, env Gene Products, Human Immunodeficiency Virus, glycan conformation, Virology, Single Molecule Imaging, antibody approach angle, HEK293 Cells, CD4 Antigens, HIV-1, biology.protein, cryo-EM, Binding Sites, Antibody, Antibody, Broadly Neutralizing Antibodies, Protein Binding

Abstract

Summary Recognition of N-linked glycan at residue N276 (glycan276) at the periphery of the CD4-binding site (CD4bs) on the HIV-envelope trimer is a formidable challenge for many CD4bs-directed antibodies. To understand how this glycan can be recognized, here we isolate two lineages of glycan276-dependent CD4bs antibodies. Antibody CH540-VRC40.01 (named for donor-lineage.clone) neutralizes 81% of a panel of 208 diverse strains, while antibody CH314-VRC33.01 neutralizes 45%. Cryo-electron microscopy (cryo-EM) structures of these two antibodies and 179NC75, a previously identified glycan276-dependent CD4bs antibody, in complex with HIV-envelope trimer reveal substantially different modes of glycan276 recognition. Despite these differences, binding of glycan276-dependent antibodies maintains a glycan276 conformation similar to that observed in the absence of glycan276-binding antibodies. By contrast, glycan276-independent CD4bs antibodies, such as VRC01, displace glycan276 upon binding. These results provide a foundation for understanding antibody recognition of glycan276 and suggest its presence may be crucial for priming immunogens seeking to initiate broad CD4bs recognition.

Published

2021

36. Paired heavy- and light-chain signatures contribute to potent SARS-CoV-2 neutralization in public antibody responses

Author

Gabriele Cerutti, Yaroslav Tsybovsky, Bharat Madan, Bailey B. Banach, Matheus Oliveira de Souza, Adam S. Olia, Tongqing Zhou, I-Ting Teng, Yaoxing Huang, Jacy R. Wolfe, Phinikoula S. Katsamba, Peter D. Kwong, Pengfei Wang, Manoj S. Nair, Timothy A. Whitehead, Chen-Hsiang Shen, Ahmed S. Fahad, David D. Ho, Kwok-Yung Yuen, Irene M. Francino-Urdaniz, Brandon J. DeKosky, Jude Bimela, Lihong Liu, Eswar R. Reddem, Amy D. Laflin, Xiaoli Pan, Rajani Nimrania, Lawrence Shapiro, Jian Yu, Alexandra Nazzari, Sheila N. Lopez Acevedo, Paul J. Steiner, Matias Gutiérrez-González, and Yang Luo

Subjects

Male, QH301-705.5, medicine.drug_class, B-cell, Computational biology, Biology, Antibodies, Viral, Immunoglobulin light chain, Monoclonal antibody, Article, General Biochemistry, Genetics and Molecular Biology, Neutralization, Immune system, Report, Chlorocebus aethiops, medicine, Animals, Humans, Protein Interaction Domains and Motifs, yeast display, Biology (General), Binding site, Vero Cells, B cell, Aged, B-Lymphocytes, Binding Sites, SARS-CoV-2, Cryoelectron Microscopy, Antibodies, Monoclonal, COVID-19, neutralization, Antibodies, Neutralizing, immunity, virology, HEK293 Cells, medicine.anatomical_structure, Antibody Formation, Spike Glycoprotein, Coronavirus, biology.protein, Immunoglobulin heavy chain, Immunoglobulin Light Chains, Angiotensin-Converting Enzyme 2, Antibody, Immunoglobulin Heavy Chains, public antibody, Protein Binding, biotechnology

Abstract

Understanding mechanisms of protective antibody recognition can inform vaccine and therapeutic strategies against SARS-CoV-2. We report a monoclonal antibody, 910-30, targeting the SARS-CoV-2 receptor-binding site for ACE2 as a member of a public antibody response encoded by IGHV3-53/IGHV3-66 genes. Sequence and structural analyses of 910-30 and related antibodies explore how class recognition features correlate with SARS-CoV-2 neutralization. Cryo-EM structures of 910-30 bound to the SARS-CoV-2 spike trimer reveal binding interactions and its ability to disassemble spike. Despite heavy-chain sequence similarity, biophysical analyses of IGHV3-53/3-66-encoded antibodies highlight the importance of native heavy:light pairings for ACE2-binding competition and SARS-CoV-2 neutralization. We develop paired heavy:light class sequence signatures and determine antibody precursor prevalence to be ∼1 in 44,000 human B cells, consistent with public antibody identification in several convalescent COVID-19 patients. These class signatures reveal genetic, structural, and functional immune features that are helpful in accelerating antibody-based medical interventions for SARS-CoV-2., Graphical abstract, Banach et al. report a SARS-CoV-2 neutralizing antibody along with genetic, structural, and functional features of public antibody responses targeting SARS-CoV-2. These data reveal how structural interactions with the SARS-CoV-2 receptor-binding domain correlate with viral neutralization and demonstrate the importance of native antibody heavy:light pairings in convergent antibody responses.

Published

2021

37. Quantification of the Impact of the HIV-1-Glycan Shield on Antibody Elicitation

Author

Michael Chambers, Chen-Hsiang Shen, Adrian B. McDermott, Barton F. Haynes, Leonidas Stamatatos, Marie Pancera, Yaroslav Tsybovsky, Diana G. Scorpio, Mark K. Louder, M. Gordon Joyce, Cinque Soto, Timothy G. Wanninger, Nicole A. Doria-Rose, Tongqing Zhou, Ivelin S. Georgiev, Baoshan Zhang, Lei Chen, Mallika Sastry, Stephen D. Schmidt, Guillaume Stewart-Jones, Rita E. Chen, Lawrence Shapiro, Peng Zhao, Reda Rawi, Kai Xu, Thomas Lemmin, Sandeep Narpala, Young Do Kwon, Sijy O'Dell, Anqi Zheng, John-Paul Todd, John R. Mascola, Krisha McKee, Peter D. Kwong, Cheng Cheng, Aliaksandr Druz, Kathryn E. Foulds, Hui Geng, Lance Wells, Yongping Yang, Gwo-Yu Chuang, Michael Tiemeyer, and S. Katie Farney

Subjects

immunogen design, 0301 basic medicine, crystal structure, Glycan, Glycosylation, glycan shield, Guinea Pigs, envelope glycoprotein, Heterologous, HIV Antibodies, Molecular Dynamics Simulation, immunogenicity, Crystallography, X-Ray, General Biochemistry, Genetics and Molecular Biology, Neutralization, Epitope, glycomics, Glycomics, Epitopes, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antibody Specificity, Polysaccharides, Animals, Humans, CD4-binding site, Protein Structure, Quaternary, lcsh:QH301-705.5, Binding Sites, biology, Immunogenicity, env Gene Products, Human Immunodeficiency Virus, targeted deglycosylation, Antibodies, Neutralizing, Macaca mulatta, Virology, carbohydrates (lipids), 030104 developmental biology, lcsh:Biology (General), chemistry, CD4 Antigens, HIV-1, vaccine design, biology.protein, Immunization, Antibody, 030217 neurology & neurosurgery

Abstract

While the HIV-1-glycan shield is known to shelter Env from the humoral immune response, its quantitative impact on antibody elicitation has been unclear. Here, we use targeted deglycosylation to measure the impact of the glycan shield on elicitation of antibodies against the CD4 supersite. We engineered diverse Env trimers with select glycans removed proximal to the CD4 supersite, characterized their structures and glycosylation, and immunized guinea pigs and rhesus macaques. Immunizations yielded little neutralization against wild-type viruses but potent CD4-supersite neutralization (titers 1: >1,000,000 against four-glycan-deleted autologous viruses with over 90% breadth against four-glycan-deleted heterologous strains exhibiting tier 2 neutralization character). To a first approximation, the immunogenicity of the glycan-shielded protein surface was negligible, with Env-elicited neutralization (ID50) proportional to the exponential of the protein-surface area accessible to antibody. Based on these high titers and exponential relationship, we propose site-selective deglycosylated trimers as priming immunogens to increase the frequency of site-targeting antibodies.

Published

2017

38. VRC34-Antibody Lineage Development Reveals How a Required Rare Mutation Shapes the Maturation of a Broad HIV-Neutralizing Lineage

Author

Bob C. Lin, John R. Mascola, Erica Normandin, Mallika Sastry, Divya Kilam, Li Ou, Shuishu Wang, Amy Ransier, Chen-Hsiang Shen, Kai Xu, Mark Connors, Mark K. Louder, Zizhang Sheng, Eric Feng, Reda Rawi, Eli Boritz, Baoshan Zhang, Brandon J. DeKosky, Rui Kong, Sung Hee Ko, Sijy O'Dell, Ying Gu, Peter D. Kwong, Kevin Liu, Gwo-Yu Chuang, Tongqing Zhou, Jesse Huang, Gunilla B. Karlsson Hedestam, Daniel C. Douek, Yiran Wang, Yicheng Guo, Stephen D. Schmidt, Lawrence Shapiro, Martin Corcoran, Cara W. Chao, and Nicole A. Doria-Rose

Subjects

Lineage (genetic), Human immunodeficiency virus (HIV), Somatic hypermutation, Gene Expression, HIV Infections, Biology, HIV Antibodies, medicine.disease_cause, Crystallography, X-Ray, Microbiology, Article, 03 medical and health sciences, 0302 clinical medicine, Virology, Rare mutations, medicine, Humans, B cell, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, B-Lymphocytes, env Gene Products, Human Immunodeficiency Virus, Antibodies, Neutralizing, medicine.anatomical_structure, Mutation testing, biology.protein, HIV-1, Parasitology, Antibody, Transcriptome, Viral Fusion Proteins, 030217 neurology & neurosurgery, Broadly Neutralizing Antibodies

Abstract

Rare mutations have been proposed to restrict the development of broadly neutralizing antibodies against HIV-1, but this has not been explicitly demonstrated. We hypothesized that such rare mutations might be identified by comparing broadly neutralizing and non-broadly neutralizing branches of an antibody-developmental tree. Because sequences of antibodies isolated from the fusion peptide (FP)-targeting VRC34-antibody lineage suggested it might be suitable for such rare mutation analysis, we carried out next-generation sequencing (NGS) on B cell transcripts from donor N123, the source of the VRC34 lineage, and functionally and structurally characterized inferred intermediates along broadly neutralizing and poorly neutralizing developmental branches. The broadly neutralizing VRC34.01 branch required the rare heavy-chain mutation Y33P to bind FP, whereas the early bifurcated VRC34.05 branch did not require this rare mutation and evolved less breadth. Our results demonstrate how a required rare mutation can restrict development and shape the maturation of a broad HIV-1-neutralizing antibody lineage.

Published

2019

39. Accurate Prediction for Antibody Resistance of Clinical HIV-1 Isolates

Author

Rebecca M. Lynch, Gwo-Yu Chuang, Peter D. Kwong, Tae-Wook Chun, Chen-Hsiang Shen, Jing Zhou, Halima Bensmail, Raghvendra Mall, Nicole A. Doria-Rose, S. Katie Farney, John R. Mascola, Reda Rawi, and Andrea Shiakolas

Subjects

Mutation rate, In silico, Human immunodeficiency virus (HIV), lcsh:Medicine, HIV Infections, Drug resistance, Biology, HIV Antibodies, medicine.disease_cause, Neutralization, Epitope, Article, Deep Learning, Immunoglobulin Idiotypes, Neutralization Tests, Machine learning, Drug Resistance, Viral, medicine, Humans, Computer Simulation, lcsh:Science, Multidisciplinary, lcsh:R, env Gene Products, Human Immunodeficiency Virus, Prognosis, Virology, Data Accuracy, Clinical trial, biology.protein, HIV-1, Infectious diseases, lcsh:Q, Binding Sites, Antibody, Antibody, Broadly Neutralizing Antibodies, Epitope Mapping

Abstract

Broadly neutralizing antibodies (bNAbs) targeting the HIV-1 envelope glycoprotein (Env) have promising utility in prevention and treatment of HIV-1 infection, and several are currently undergoing clinical trials. Due to the high sequence diversity and mutation rate of HIV-1, viral isolates are often resistant to specific bNAbs. Currently, resistant isolates are commonly identified by time-consuming and expensive in vitro neutralization assays. Here, we report machine learning classifiers that accurately predict resistance of HIV-1 isolates to 33 bNAbs. Notably, our classifiers achieved an overall prediction accuracy of 96% for 212 clinical isolates from patients enrolled in four different clinical trials. Moreover, use of gradient boosting machine – a tree-based machine learning method – enabled us to identify critical features, which had high accordance with epitope residues that distinguished between antibody resistance and sensitivity. The availability of an in silico antibody resistance predictor should facilitate informed decisions of antibody usage and sequence-based monitoring of viral escape in clinical settings.

Published

2019

40. Structure of Super-Potent Antibody CAP256-VRC26.25 in Complex with HIV-1 Envelope Reveals a Combined Mode of Trimer-Apex Recognition

Author

John R. Mascola, Aliaksandr Druz, Nicole A. Doria-Rose, Jason Gorman, Bob C. Lin, Krisha McKee, Raffaello Verardi, Yongping Yang, Peter D. Kwong, Reda Rawi, Penny L. Moore, Lawrence Shapiro, Hui Geng, Lynn Morris, Jeffrey C. Boyington, Gwo-Yu Chuang, Chen-Hsiang Shen, Mark K. Louder, Baoshan Zhang, and Yen-Ting Lai

Subjects

0301 basic medicine, Tyrosine sulfation, Lineage (genetic), Broadly neutralizing antibody, Trimer, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Hiv 1 envelope, General Biochemistry, Genetics and Molecular Biology, Cell Line, 03 medical and health sciences, Immunoglobulin Fab Fragments, 0302 clinical medicine, Humans, Antibody Classes, Amino Acid Sequence, lcsh:QH301-705.5, biology, Chemistry, Cryoelectron Microscopy, env Gene Products, Human Immunodeficiency Virus, Antibodies, Neutralizing, Apex (geometry), Cell biology, 030104 developmental biology, lcsh:Biology (General), biology.protein, HIV-1, Antibody, Protein Multimerization, 030217 neurology & neurosurgery, Protein Binding

Abstract

Summary: Antibodies targeting the V1V2 apex of the HIV-1 envelope (Env) trimer comprise one of the most commonly elicited categories of broadly neutralizing antibodies. Structures of these antibodies indicate diverse modes of Env recognition typified by antibodies of the PG9 class and the PGT145 class. The mode of recognition, however, has been unclear for the most potent of the V1V2 apex-targeting antibodies, CAP256-VRC26.25 (named for donor-lineage.clone and referred to hereafter as VRC26.25). Here, we determine the cryoelectron microscopy structure at 3.7 Å resolution of the antigen-binding fragment of VRC26.25 in complex with the Env trimer thought to have initiated the lineage. The 36-residue protruding loop of VRC26.25 displays recognition incorporating both strand-C interactions similar to the PG9 class and V1V2 apex insertion similar to the PGT145 class. Structural elements of separate antibody classes can thus intermingle to form a “combined” class, which in this case yields an antibody of extraordinary potency. : Antibody CAP256-VRC26.25 is one of the most potent known HIV-1-neutralizing antibodies. Gorman et al. determine the cryo-EM structure of this antibody in complex with the Env trimer that initiated the antibody lineage. The structure reveals how elements of distinct antibody classes can intermingle to yield an antibody of extraordinary potency. Keywords: broadly neutralizing antibody, HIV-1 envelope trimer, multidonor antibody class, PCT64, PG9, PGDM1400, PGT145, tyrosine sulfation, V1V2 apex recognition

Published

2019

41. Longitudinal Analysis Reveals Early Development of Three MPER-Directed Neutralizing Antibody Lineages from an HIV-1-Infected Individual

Author

Baoshan Zhang, Peter D. Kwong, Yen-Ting Lai, Raffaello Verardi, Moody, Annemarie O'Sullivan, Sodsai Tovanabutra, Gwo-Yu Chuang, Krisha McKee, Reda Rawi, Andrea Shiakolas, Daniel C. Douek, Merlin L. Robb, Evan M. Cale, Alberto Cagigi, John R. Mascola, Vincent Dussupt, L. Mendez, Tyler Stephens, Yaroslav Tsybovsky, Morgane Rolland, Tongqing Zhou, Chen-Hsiang Shen, Chaim A. Schramm, W.H. Law, Adrian B. McDermott, S. Gift, Jonathan R. McDaniel, Mark K. Louder, Eric Sanders-Buell, C. Tucker, Shelly J. Krebs, Meera Bose, Mangaiarkarasi Asokan, Young Do Kwon, Marissa C. Jarosinski, Nicole A. Doria-Rose, Agnès-Laurence Chenine, Barton F. Haynes, Jason Gorman, Lawrence Shapiro, Farida Laboune, J.I. Driscoll, Christopher L. Owen, S.M. Alam, Sam Darko, Robert T. Bailer, D. Peng, Kenneth H. Zhou, Sebastian Schätzle, Ivelin S. Georgiev, Nelson L. Michael, George Georgiou, Mallika Sastry, Victoria R. Polonis, K. Wang, Jing Zhou, Gina Donofrio, Gary R. Matyas, Amy Ransier, and Aliaksandr Druz

Subjects

0301 basic medicine, Immunogen, Lineage (evolution), Immunology, Somatic hypermutation, HIV Infections, Biology, HIV Antibodies, Neutralization, Virus, Article, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunology and Allergy, Humans, Amino Acid Sequence, Longitudinal Studies, Neutralizing antibody, AIDS Vaccines, B-Lymphocytes, Virology, Antibodies, Neutralizing, 030104 developmental biology, Infectious Diseases, HEK293 Cells, 030220 oncology & carcinogenesis, biology.protein, HIV-1, Leukocytes, Mononuclear, Antibody

Abstract

Summary Lineage-based vaccine design is an attractive approach for eliciting broadly neutralizing antibodies (bNAbs) against HIV-1. However, most bNAb lineages studied to date have features indicative of unusual recombination and/or development. From an individual in the prospective RV217 cohort, we identified three lineages of bNAbs targeting the membrane-proximal external region (MPER) of the HIV-1 envelope. Antibodies RV217-VRC42.01, -VRC43.01, and -VRC46.01 used distinct modes of recognition and neutralized 96%, 62%, and 30%, respectively, of a 208-strain virus panel. All three lineages had modest levels of somatic hypermutation and normal antibody-loop lengths and were initiated by the founder virus MPER. The broadest lineage, VRC42, was similar to the known bNAb 4E10. A multimeric immunogen based on the founder MPER activated B cells bearing the unmutated common ancestor of VRC42, with modest maturation of early VRC42 intermediates imparting neutralization breadth. These features suggest that VRC42 may be a promising template for lineage-based vaccine design.

Published

2019

42. Structure of Antibody CAP256-VRC26.25 in Complex with HIV-1 Envelope Reveals a Combined Mode of Trimer-Apex Recognition

Author

Chen-Hsiang Shen, Krisha McKee, Peter D. Kwong, Mark K. Louder, Raffaello Verardi, Yongping Yang, Reda Rawi, John R. Mascola, Baoshan Zhang, Yen-Ting Lai, Gwo-Yu Chuang, Penny L. Moore, Lawrence Shapiro, Aliaksandr Druz, Nicole A. Doria-Rose, Jason Gorman, Bob C. Lin, Hui Geng, Lynn Morris, and Jeffrey C. Boyington

Subjects

Tyrosine sulfation, Lineage (genetic), biology, Chemistry, Broadly neutralizing antibody, biology.protein, Trimer, Antibody Classes, Antibody, Hiv 1 envelope, Cell biology

Abstract

Antibodies targeting the V1V2-apex of the HIV-1 envelope (Env) trimer comprise one of the most commonly elicited categories of broadly neutralizing antibodies. Structures of these antibodies indicate diverse modes of Env recognition typified by antibodies of the PG9 class and the PGT145 class. The mode of recognition, however, has been unclear for the most potent of the V1V2-apex-targeting antibodies, CAP256-VRC26.25 (named for donor-lineage.clone). Here we determine the cryo-electron microscopy structure at 3.8-A resolution of the antigen-binding fragment of CAP256-VRC26.25 in complex with the Env trimer thought to have initiated the lineage. Remarkably, the 36-residue protruding loop of CAP256-VRC26.25 displayed recognition incorporating both strand-C interactions similar to the PG9 class and V1V2-apex insertion similar to the PGT145 class. Structural elements of separate antibody classes can thus intermingle to form a “combined” class, which in this case yields an antibody of extraordinary potency.

Published

2019

43. Vaccination with prefusion-stabilized respiratory syncytial virus fusion protein induces genetically and antigenically diverse antibody responses

Author

Nancy J. Sullivan, Bharat Madan, Emily Phung, John R. Mascola, Barney S. Graham, Chaim A. Schramm, Daniel Wrapp, Jason S. McLellan, Tracy J. Ruckwardt, Daniel C. Douek, John Misasi, Nicole A. Doria-Rose, Lingshu Wang, Pamela Costner, Guillaume Stewart-Jones, Samuel Darko, Maryam Mukhamedova, Amy Ransier, Chen-Hsiang Shen, Martin R. Gaudinski, Sarah A.M. Lucas, Peter D. Kwong, Larissa Ault, Morgan S.A. Gilman, Somia P. Hickman, Yi Zhang, Nina M. Berkowitz, Brandon J. DeKosky, Grace L. Chen, LaSonji A. Holman, Scott A. Rush, Alexandrine Derrien-Colemyn, Kaitlyn M. Morabito, Michelle C. Crank, and Lauren A. Chang

Subjects

Adult, Male, 0301 basic medicine, Adolescent, Immunology, Respiratory Syncytial Virus Infections, Antibodies, Viral, Article, Epitope, Virus, Cell Line, Cohort Studies, Epitopes, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Antibody Repertoire, Antigen, Cell Line, Tumor, Respiratory Syncytial Virus Vaccines, Humans, Immunology and Allergy, Child, Aged, Aged, 80 and over, biology, Vaccination, Infant, Newborn, Infant, Middle Aged, Antibodies, Neutralizing, Fusion protein, Virology, HEK293 Cells, 030104 developmental biology, Infectious Diseases, Polyclonal B cell response, Child, Preschool, Respiratory Syncytial Virus, Human, 030220 oncology & carcinogenesis, Antibody Formation, biology.protein, Female, Antibody, Viral Fusion Proteins

Abstract

An effective vaccine for respiratory syncytial virus (RSV) is an unrealized public health goal. A single dose of the prefusion-stabilized fusion (F) glycoprotein subunit vaccine (DS-Cav1) substantially increases serum-neutralizing activity in healthy adults. We sought to determine whether DS-Cav1 vaccination induces a repertoire mirroring the pre-existing diversity from natural infection or whether antibody lineages targeting specific epitopes predominate. We evaluated RSV F-specific B cell responses before and after vaccination in six participants using complementary B cell sequencing methodologies and identified 555 clonal lineages. DS-Cav1-induced lineages recognized the prefusion conformation of F (pre-F) and were genetically diverse. Expressed antibodies recognized all six antigenic sites on the pre-F trimer. We identified 34 public clonotypes, and structural analysis of two antibodies from a predominant clonotype revealed a common mode of recognition. Thus, vaccination with DS-Cav1 generates a diverse polyclonal response targeting the antigenic sites on pre-F, supporting the development and advanced testing of pre-F-based vaccines against RSV.

Published

2021

44. Vaccination induces maturation in a mouse model of diverse unmutated VRC01-class precursors to HIV-neutralizing antibodies with >50% breadth

Author

Nicole A. Doria-Rose, Ying Gu, Peter D. Kwong, Zizhang Sheng, John R. Mascola, Cheng Cheng, Michelle X. Zheng, Xuejun Chen, Gwo-Yu Chuang, Ming Tian, Hongying Duan, Tongqing Zhou, Stephen D. Schmidt, Lawrence Shapiro, Bob C. Lin, Chen-Hsiang Shen, Mark K. Louder, Frederick W. Alt, and M. Gordon Joyce

Subjects

0301 basic medicine, Glycan, Immunology, Human immunodeficiency virus (HIV), Somatic hypermutation, HIV Infections, Mice, Transgenic, HIV Antibodies, Lymphocyte Activation, medicine.disease_cause, Article, Neutralization, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Immunology and Allergy, AIDS Vaccines, B-Lymphocytes, biology, Hiv 1 vaccine, Vaccination, Virology, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Infectious Diseases, Immunization, 030220 oncology & carcinogenesis, Mutation, HIV-1, biology.protein, Somatic Hypermutation, Immunoglobulin, Antibody, Broadly Neutralizing Antibodies

Abstract

Vaccine elicitation of broadly neutralizing antibodies (bnAbs) is a key HIV-research goal. The VRC01 class of bnAbs targets the CD4-binding site on the HIV-envelope trimer and requires extensive somatic hypermutation (SHM) to neutralize effectively. Despite substantial progress, vaccine-induced VRC01-class antibodies starting from unmutated precursors have exhibited limited neutralization breadth, particularly against viruses bearing glycan on loop D residue N276 (glycan276), present on most circulating strains. Here, using sequential immunization of immunoglobulin (Ig)-humanized mice expressing diverse unmutated VRC01-class antibody precursors, we elicited serum responses capable of neutralizing viruses bearing glycan276 and isolated multiple lineages of VRC01-class bnAbs, including two with >50% breadth on a 208-strain panel. Crystal structures of representative bnAbs revealed the same mode of recognition as known VRC01-class bnAbs. Structure-function studies further pinpointed key mutations and correlated their induction with specific immunizations. VRC01-class bnAbs can thus be matured by sequential immunization from unmutated ancestors to >50% breadth, and we delineate immunogens and regimens inducing key SHM.

Published

2021

45. Vaccine-Induced Antibodies that Neutralize Group 1 and Group 2 Influenza A Viruses

Author

Celia Santos, Peter D. Kwong, Wing-Pui Kong, Baoshan Zhang, Yi Zhang, Amy Ransier, Robert T. Bailer, Kwanyee Leung, Richard A. Koup, Sam Darko, Tatsiana Bylund, Sandeep N. Narpala, Hadi M. Yassine, Ulrich Baxa, Cinque Soto, Rebecca A. Gillespie, M. Gordon Joyce, Julie E. Ledgerwood, Xueling Wu, Lawrence Shapiro, Madhu Prabhakaran, Adam K. Wheatley, Ivelin S. Georgiev, Kanta Subbarao, Chen-Hsiang Shen, Adrian B. McDermott, Gwo-Yu Chuang, Yumiko Matsuoka, Mangaiarkarasi Asokan, James C. Mullikin, Yaroslav Tsybovsky, Lingshu Wang, Paul V. Thomas, Jeffrey C. Boyington, Aliaksandr Druz, James R R Whittle, Daniel C. Douek, Eun Sung Yang, Mario Roederer, Masaru Kanekiyo, John R. Mascola, Barney S. Graham, and Christopher R. Lees

Subjects

0301 basic medicine, biology, Influenza vaccine, Hemagglutinin (influenza), medicine.disease_cause, Virology, H5N1 genetic structure, Influenza, General Biochemistry, Genetics and Molecular Biology, Influenza A virus subtype H5N1, Epitope, Vaccination, 03 medical and health sciences, 030104 developmental biology, Immunization, biology.protein, medicine, Antibody, Vaccine

Abstract

Antibodies capable of neutralizing divergent influenza A viruses could form the basis of a universal vaccine. Here, from subjects enrolled in an H5N1 DNA/MIV-prime-boost influenza vaccine trial, we sorted hemagglutinin cross-reactive memory B cells and identified three antibody classes, each capable of neutralizing diverse subtypes of group 1 and group 2 influenza A viruses. Co-crystal structures with hemagglutinin revealed that each class utilized characteristic germline genes and convergent sequence motifs to recognize overlapping epitopes in the hemagglutinin stem. All six analyzed subjects had sequences from at least one multidonor class, and—in half the subjects—multidonor-class sequences were recovered from >40% of cross-reactive B cells. By contrast, these multidonor-class sequences were rare in published antibody datasets. Vaccination with a divergent hemagglutinin can thus increase the frequency of B cells encoding broad influenza A-neutralizing antibodies. We propose the sequence signature-quantified prevalence of these B cells as a metric to guide universal influenza A immunization strategies.

Published

2016

46. Role of humoral immunity against hepatitis B virus core antigen in the pathogenesis of acute liver failure

Author

Ronald E. Engle, David E. Kleiner, Fausto Zamboni, Kevin W. Bock, Davide De Battista, Juraj Kabat, Cinque Soto, Patrizia Farci, Sugantha Govindarajan, Zhifeng Long, Robert H. Purcell, Giacomo Diaz, Huaying Zhao, Zhaochun Chen, Chen-Hsiang Shen, Ian N. Moore, Teresa Pollicino, Peter D. Kwong, Peter Schuck, and Kurt Wollenberg

Subjects

Adult, Male, 0301 basic medicine, Hepatitis B virus, Pan troglodytes, acute liver failure, hepatitis B core antigen, hepatitis B virus, humoral immunity, pathogenesis, T-Lymphocytes, medicine.medical_treatment, Liver transplantation, Biology, Antibodies, Viral, medicine.disease_cause, Virus, 03 medical and health sciences, 0302 clinical medicine, Antigen, medicine, Animals, Humans, B cell, B-Lymphocytes, Multidisciplinary, virus diseases, Liver Failure, Acute, Middle Aged, Hepatitis B, Hepatitis B Core Antigens, Virology, digestive system diseases, Immunity, Humoral, HBcAg, 030104 developmental biology, medicine.anatomical_structure, Liver, PNAS Plus, Viral replication, Humoral immunity, Female, 030211 gastroenterology & hepatology

Abstract

Hepatitis B virus (HBV)-associated acute liver failure (ALF) is a dramatic clinical syndrome leading to death or liver transplantation in 80% of cases. Due to the extremely rapid clinical course, the difficulties in obtaining liver specimens, and the lack of an animal model, the pathogenesis of ALF remains largely unknown. Here, we performed a comprehensive genetic and functional characterization of the virus and the host in liver tissue from HBV-associated ALF and compared the results with those of classic acute hepatitis B in chimpanzees. In contrast with acute hepatitis B, HBV strains detected in ALF livers displayed highly mutated HBV core antigen (HBcAg), associated with increased HBcAg expression ex vivo, which was independent of viral replication levels. Combined gene and miRNA expression profiling revealed a dominant B cell disease signature, with extensive intrahepatic production of IgM and IgG in germline configuration exclusively targeting HBcAg with subnanomolar affinities, and complement deposition. Thus, HBV ALF appears to be an anomalous T cell-independent, HBV core-driven B cell disease, which results from the rare and unfortunate encounter between a host with an unusual B cell response and an infecting virus with a highly mutated core antigen.

Published

2018

47. CRISPro: An Automated Pipeline for Protein Conformation Stabilization by Proline

Author

Chen-Hsiang Shen, Reda Rawi, Gwo-Yu Chuang, and Peter D. Kwong

Subjects

Steric effects, Models, Molecular, Antigenicity, Immunogen, Proline, Stereochemistry, Protein Conformation, General Chemical Engineering, Library and Information Sciences, Protein Engineering, Protein Structure, Secondary, Workflow, Viral Proteins, Protein structure, Protein stability, Humans, Protein secondary structure, Chemistry, Protein Stability, Proteins, General Chemistry, Protein engineering, Computer Science Applications, Mutation, Software

Abstract

Recent studies have shown that the yield, antigenicity, and immunogenicity of an immunogen can be enhanced by stabilizing it into a specific conformation. Such stabilization often involves the engineering of proline mutations at residue positions where a proline is structurally compatible with the target conformation but not with an alternative conformation. However, there is no publicly available tool that can design proline mutations for this purpose automatically. Here we implemented an automated tool, CRISPro, that inputs structural coordinates of the target conformation and/or an alternative conformation and outputs a list of residue positions where proline mutations are predicted to stabilize the target conformation based on compatibility of phi-psi angles, secondary structure, and steric constraints. Thus, CRISPro can be used to engineer immunogens into specific conformation and to design serologic probes, capable of isolating antibodies that recognize a target shape.

Published

2018

48. Accurate Prediction of Antibody Resistance in Clinical HIV-1 Isolates

Author

Andrea Shiakolas, Raghvendra Mall, Reda Rawi, Chen-Hsiang Shen, Nicole A. Doria-Rose, John R. Mascola, Gwo-Yu Chuang, S. Katie Farney, Rebecca M. Lynch, Peter D. Kwong, Tae-Wook Chun, and Jing Zhou

Subjects

Clinical trial, Mutation rate, In silico, biology.protein, Human immunodeficiency virus (HIV), medicine, Clinical settings, Biology, Antibody, medicine.disease_cause, Virology, Epitope, Neutralization

Abstract

Broadly neutralizing antibodies (bNAbs) targeting the HIV-1 envelope glycoprotein (Env) have promising utility in prevention and treatment of HIV-1 infection with several undergoing clinical trials. Due to high sequence diversity and mutation rate of HIV-1, viral isolates are often resistant to particular bNAbs. Resistant strains are commonly identified by time-consuming and expensive in vitro neutralization experiments. Here, we developed machine learning-based classifiers that accurately predict resistance of HIV-1 strains to 33 neutralizing antibodies. Notably, our classifiers achieved an overall prediction accuracy of 96% for 212 clinical isolates from patients enrolled in four different clinical trials. Moreover, use of the tree-based machine learning method gradient boosting machine enabled us to identify critical epitope features that distinguish between antibody resistance and sensitivity. The availability of an in silico antibody resistance predictor will facilitate informed decisions of antibody usage in clinical settings.

Published

2018

49. Structural survey of HIV-1-neutralizing antibodies targeting Env trimer delineates epitope categories and suggests vaccine templates

Author

Anthony P. West, Jing Zhou, Krisha McKee, Lucy Shapiro, Reda Rawi, Gwo-Yu Chuang, Robert T. Bailer, Peter D. Kwong, Mascola, Zizhang Sheng, Pamela J. Bjorkman, Tongqing Zhou, Chen-Hsiang Shen, Mark K. Louder, Nicole A. Doria-Rose, and Baoshan Zhang

Subjects

chemistry.chemical_compound, Glycosylation, chemistry, biology, Protein subunit, Protein Data Bank (RCSB PDB), biology.protein, Somatic hypermutation, Paratope, Antibody, Virology, Neutralization, Epitope

Abstract

HIV-1 broadly neutralizing antibodies are desired for their therapeutic potential and as templates for vaccine design. Such antibodies target the HIV-1-envelope (Env) trimer, which is shielded from immune recognition by extraordinary glycosylation and sequence variability. Recognition by broadly neutralizing antibodies thus provides insight into how antibody can bypass these immune-evasion mechanisms. Remarkably, antibodies neutralizing >25% of HIV-1 strains have now been identified that recognize all major exposed surfaces of the prefusion-closed Env trimer. Here we analyzed all 206 broadly neutralizing antibody-HIV-1 Env complexes in the PDB with resolution suitable to define their interaction chemistries. These segregated into 20 antibody classes based on ontogeny and recognition, and into 6 epitope categories (V1V2, glycan-V3, CD4-binding site, silent face center, fusion peptide, andsubunit interface) based on recognized Env residues. We measured antibody neutralization on a 208-isolate panel and analyzed features of paratope and B cell ontogeny. The number of protruding loops, CDR H3 length, and level of somatic hypermutation for broadly HIV-1 neutralizing antibodies were significantly higher than for a comparison set of non-HIV-1 antibodies. For epitope, the number of independent sequence segments was higher (P < 0.0001), as well as the glycan component surface area (P = 0.0005). Based on B cell ontogeny, paratope, and breadth, the CD4-binding site antibody IOMA appeared to be a promising candidate for lineage-based vaccine design. In terms of epitope-based vaccine design, antibody VRC34.01 had few epitope segments, low epitope-glycan content, and high epitope-conformational variability, which may explain why VRC34.01-based design is yielding promising vaccine results.

Published

2018

50. Epitope-based vaccine design yields fusion peptide-directed antibodies that neutralize diverse strains of HIV-1

Author

Diana G. Scorpio, Clint Potter, Rui Kong, Reda Rawi, Robert T. Bailer, Alexander J. Jafari, Cheng Cheng, Rui Chen, Hui Geng, Nicole A. Doria-Rose, Chen-Hsiang Shen, Adrian B. McDermott, Kevin Liu, Mark K. Louder, Li Ou, Venkata P. Dandey, Peter D. Kwong, Baoshan Zhang, Yen-Ting Lai, Yaohui Wang, Mangaiarkarasi Asokan, Young Do Kwon, Kurt R. Hill, Ariana P. Rowshan, John Paul Todd, Ivelin S. Georgiev, Mallika Sastry, Yaroslav Tsybovsky, Krisha McKee, Michael Chambers, Xuejun Chen, Sijy O'Dell, A.F. Zhou, Hui Wei, S.K. Farney, John R. Mascola, Zizhang Sheng, Kathryn E. Foulds, Tongqing Zhou, L. Yang, Thomas Lemmin, Kai Xu, Edward T. Eng, Jason Gorman, Gwo-Yu Chuang, Chang W. Choi, Bridget Carragher, E.G. Viox, Lawrence Shapiro, T.Y. Ohr, Priyamvada Acharya, Aliaksandr Druz, Yongping Yang, and Dongjun Peng

Subjects

0301 basic medicine, Models, Molecular, Viral protein, medicine.drug_class, Recombinant Fusion Proteins, Guinea Pigs, Peptide, HIV Antibodies, medicine.disease_cause, Monoclonal antibody, General Biochemistry, Genetics and Molecular Biology, Epitope, Neutralization, 03 medical and health sciences, Epitopes, 0302 clinical medicine, Immune system, Viral entry, Neutralization Tests, medicine, Animals, Amino Acid Sequence, HIV vaccine, 030304 developmental biology, chemistry.chemical_classification, AIDS Vaccines, 0303 health sciences, biology, env Gene Products, Human Immunodeficiency Virus, General Medicine, Virology, Antibodies, Neutralizing, Macaca mulatta, 3. Good health, Mice, Inbred C57BL, 030104 developmental biology, Immunization, chemistry, biology.protein, HIV-1, Female, Antibody, Peptides, 030217 neurology & neurosurgery

Abstract

A central goal of HIV-1 vaccine research is the elicitation of antibodies capable of neutralizing diverse primary isolates of HIV-1. Here we show that focusing the immune response to exposed N-terminal residues of the fusion peptide, a critical component of the viral entry machinery and the epitope of antibodies elicited by HIV-1 infection, through immunization with fusion peptide-coupled carriers and prefusion stabilized envelope trimers, induces cross-clade neutralizing responses. In mice, these immunogens elicited monoclonal antibodies capable of neutralizing up to 31% of a cross-clade panel of 208 HIV-1 strains. Crystal and cryoelectron microscopy structures of these antibodies revealed fusion peptide conformational diversity as a molecular explanation for the cross-clade neutralization. Immunization of guinea pigs and rhesus macaques induced similarly broad fusion peptide-directed neutralizing responses, suggesting translatability. The N terminus of the HIV-1 fusion peptide is thus a promising target of vaccine efforts aimed at eliciting broadly neutralizing antibodies. An alternative HIV vaccine design facilitates generation of HIV-1-antibodies, with promising neutralization breadth in rodents and nonhuman primates.

Published

2018