Your search keyword '"Edward F. Kreider"' showing total 18 results

1. Effective treatment of SIVcpz-induced immunodeficiency in a captive western chimpanzee

Author

Hannah J. Barbian, Raven Jackson-Jewett, Corrine S. Brown, Frederic Bibollet-Ruche, Gerald H. Learn, Timothy Decker, Edward F. Kreider, Yingying Li, Thomas N. Denny, Paul M. Sharp, George M. Shaw, Jeffrey Lifson, Edward P. Acosta, Michael S. Saag, Katharine J. Bar, and Beatrice H. Hahn

Subjects

SIVcpz, Chimpanzees, Antiretroviral therapy, AIDS, Drug resistance, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Background Simian immunodeficiency virus of chimpanzees (SIVcpz), the progenitor of human immunodeficiency virus type 1 (HIV-1), is associated with increased mortality and AIDS-like immunopathology in wild-living chimpanzees (Pan troglodytes). Surprisingly, however, similar findings have not been reported for chimpanzees experimentally infected with SIVcpz in captivity, raising questions about the intrinsic pathogenicity of this lentivirus. Findings Here, we report progressive immunodeficiency and clinical disease in a captive western chimpanzee (P. t. verus) infected twenty years ago by intrarectal inoculation with an SIVcpz strain (ANT) from a wild-caught eastern chimpanzee (P. t. schweinfurthii). With sustained plasma viral loads of 105 to 106 RNA copies/ml for the past 15 years, this chimpanzee developed CD4+ T cell depletion (220 cells/μl), thrombocytopenia (90,000 platelets/μl), and persistent soft tissue infections refractory to antibacterial therapy. Combination antiretroviral therapy consisting of emtricitabine (FTC), tenofovir disoproxil fumarate (TDF), and dolutegravir (DTG) decreased plasma viremia to undetectable levels (

Published

2017

2. Completeness of HIV-1 Envelope Glycan Shield at Transmission Determines Neutralization Breadth

Author

Kshitij Wagh, Edward F. Kreider, Yingying Li, Hannah J. Barbian, Gerald H. Learn, Elena Giorgi, Peter T. Hraber, Timothy G. Decker, Andrew G. Smith, Marcos V. Gondim, Lindsey Gillis, Jamie Wandzilak, Gwo-Yu Chuang, Reda Rawi, Fangping Cai, Pierre Pellegrino, Ian Williams, Julie Overbaugh, Feng Gao, Peter D. Kwong, Barton F. Haynes, George M. Shaw, Persephone Borrow, Michael S. Seaman, Beatrice H. Hahn, and Bette Korber

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Densely arranged N-linked glycans shield the HIV-1 envelope (Env) trimer from antibody recognition. Strain-specific breaches in this shield (glycan holes) can be targets of vaccine-induced neutralizing antibodies that lack breadth. To understand the interplay between glycan holes and neutralization breadth in HIV-1 infection, we developed a sequence- and structure-based approach to identify glycan holes for individual Env sequences that are shielded in most M-group viruses. Applying this approach to 12 longitudinally followed individuals, we found that transmitted viruses with more intact glycan shields correlated with development of greater neutralization breadth. Within 2 years, glycan acquisition filled most glycan holes present at transmission, indicating escape from hole-targeting neutralizing antibodies. Glycan hole filling generally preceded the time to first detectable breadth, although time intervals varied across hosts. Thus, completely glycan-shielded viruses were associated with accelerated neutralization breadth development, suggesting that Env immunogens with intact glycan shields may be preferred components of AIDS vaccines. : Wagh et al. show that transmitted viruses with more intact glycan shields are correlated with development of neutralization breadth in HIV-1-infected individuals. This is consistent with previous findings that glycan holes in Env immunogens are targeted by strain-specific neutralizing responses, and suggests that immunogens with intact glycan shields may be advantageous. Keywords: neutralizing antibodies, glycan shield, HIV-1 envelope, transmitted founder, vaccine design

Published

2018

3. Longitudinal Antigenic Sequences and Sites from Intra-Host Evolution (LASSIE) Identifies Immune-Selected HIV Variants

Author

Peter Hraber, Bette Korber, Kshitij Wagh, Elena E. Giorgi, Tanmoy Bhattacharya, S. Gnanakaran, Alan S. Lapedes, Gerald H. Learn, Edward F. Kreider, Yingying Li, George M. Shaw, Beatrice H. Hahn, David C. Montefiori, S. Munir Alam, Mattia Bonsignori, M. Anthony Moody, Hua-Xin Liao, Feng Gao, and Barton F. Haynes

Subjects

human immunodeficiency virus type 1, vaccine, neutralizing antibodies, immunogen design, envelope glycoprotein, coevolution, immune escape, quasispecies, antigenic swarm, selection, Microbiology, QR1-502

Abstract

Within-host genetic sequencing from samples collected over time provides a dynamic view of how viruses evade host immunity. Immune-driven mutations might stimulate neutralization breadth by selecting antibodies adapted to cycles of immune escape that generate within-subject epitope diversity. Comprehensive identification of immune-escape mutations is experimentally and computationally challenging. With current technology, many more viral sequences can readily be obtained than can be tested for binding and neutralization, making down-selection necessary. Typically, this is done manually, by picking variants that represent different time-points and branches on a phylogenetic tree. Such strategies are likely to miss many relevant mutations and combinations of mutations, and to be redundant for other mutations. Longitudinal Antigenic Sequences and Sites from Intrahost Evolution (LASSIE) uses transmitted founder loss to identify virus “hot-spots” under putative immune selection and chooses sequences that represent recurrent mutations in selected sites. LASSIE favors earliest sequences in which mutations arise. With well-characterized longitudinal Env sequences, we confirmed selected sites were concentrated in antibody contacts and selected sequences represented diverse antigenic phenotypes. Practical applications include rapidly identifying immune targets under selective pressure within a subject, selecting minimal sets of reagents for immunological assays that characterize evolving antibody responses, and for immunogens in polyvalent “cocktail” vaccines.

Published

2015

4. HIV-1 Reservoir Persistence and Decay: Implications for Cure Strategies

Author

Edward F. Kreider and Katharine J. Bar

Subjects

Infectious Diseases, Virology

Published

2022

5. HIV-1 Neutralizing Antibody Signatures and Application to Epitope-Targeted Vaccine Design

Author

Christine A. Bricault, Karina Yusim, Michael S. Seaman, Hyejin Yoon, James Theiler, Elena E. Giorgi, Kshitij Wagh, Maxwell Theiler, Peter Hraber, Jennifer P. Macke, Edward F. Kreider, Gerald H. Learn, Beatrice H. Hahn, Johannes F. Scheid, James M. Kovacs, Jennifer L. Shields, Christy L. Lavine, Fadi Ghantous, Michael Rist, Madeleine G. Bayne, George H. Neubauer, Katherine McMahan, Hanqin Peng, Coraline Chéneau, Jennifer J. Jones, Jie Zeng, Christina Ochsenbauer, Joseph P. Nkolola, Kathryn E. Stephenson, Bing Chen, S. Gnanakaran, Mattia Bonsignori, LaTonya D. Williams, Barton F. Haynes, Nicole Doria-Rose, John R. Mascola, David C. Montefiori, Dan H. Barouch, and Bette Korber

Subjects

Models, Molecular, signature analysis, Guinea Pigs, V2-apex antibodies, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Microbiology, Article, Epitopes, Inhibitory Concentration 50, Virology, Animals, Humans, Amino Acid Sequence, Vaccines, broadly neutralizing antibodies, Vaccination, env Gene Products, Human Immunodeficiency Virus, virus diseases, Antibodies, Neutralizing, Peptide Fragments, Disease Models, Animal, machine learning, HEK293 Cells, Antibody Formation, Mutation, vaccine design, HIV-1, Parasitology, Female, Immunization, hypervariable regions, Protein Binding

Abstract

Summary Eliciting HIV-1-specific broadly neutralizing antibodies (bNAbs) remains a challenge for vaccine development, and the potential of passively delivered bNAbs for prophylaxis and therapeutics is being explored. We used neutralization data from four large virus panels to comprehensively map viral signatures associated with bNAb sensitivity, including amino acids, hypervariable region characteristics, and clade effects across four different classes of bNAbs. The bNAb signatures defined for the variable loop 2 (V2) epitope region of HIV-1 Env were then employed to inform immunogen design in a proof-of-concept exploration of signature-based epitope targeted (SET) vaccines. V2 bNAb signature-guided mutations were introduced into Env 459C to create a trivalent vaccine, and immunization of guinea pigs with V2-SET vaccines resulted in increased breadth of NAb responses compared with Env 459C alone. These data demonstrate that bNAb signatures can be utilized to engineer HIV-1 Env vaccine immunogens capable of eliciting antibody responses with greater neutralization breadth., Graphical Abstract, Highlights • HIV-1 bNAb sensitivity signatures from 4 large virus panels mapped across 4 Ab classes • Non-contact hypervariable region characteristics are critical for bNAb sensitivity • HIV-1 Env 459C used alone as a vaccine can elicit modest tier 2 NAbs in guinea pigs • V2 bNAb signature-guided modifications in 459C enhanced neutralization breadth, HIV-1 Env amino acid signatures associated with sensitivity to broadly neutralizing antibodies were systematically defined from large neutralization panels. V2 signatures were incorporated in a trivalent vaccine to enhance epitope exposure and to include common epitope variants, resulting in increased neutralization breadth against heterologous viruses in a guinea pig model.

Published

2018

6. Comparing medical, dental, and nursing students' preparedness to address lesbian, gay, bisexual, transgender, and queer health

Author

Madelyne Z. Greene, Katherine France, Edward F. Kreider, Emily Wolfe-Roubatis, Kevin D. Chen, Andy Wu, and Baligh R. Yehia

Subjects

Male, Students, Medical, Health Care Providers, Students, Dental, Social Sciences, lcsh:Medicine, Surveys, Sexual and Gender Minorities, 0302 clinical medicine, Sociology, Surveys and Questionnaires, Transgender, Health care, Medicine and Health Sciences, 030212 general & internal medicine, lcsh:Science, Allied Health Care Professionals, Multidisciplinary, Schools, 4. Education, Health equity, 3. Good health, Health Education and Awareness, Research Design, Health, Preparedness, Female, Lesbian, Psychology, Research Article, Adult, Full-time, Attitude of Health Personnel, Oral Medicine, education, MEDLINE, Research and Analysis Methods, Education, 03 medical and health sciences, Nursing Science, Young Adult, Nursing, Humans, Demography, Survey Research, business.industry, lcsh:R, 030206 dentistry, Health Care, Logistic Models, Medical Education, Students, Nursing, lcsh:Q, business, Oral medicine, Medical Humanities

Abstract

Background Lesbian, gay, bisexual, transgender, and queer (LGBTQ) populations face multiple health disparities including barriers to healthcare. Few studies have examined healthcare trainees’ perceptions of their preparedness to care for LGBTQ populations and none have compared perceptions of training across medicine, dental medicine, and nursing. We aimed to understand variations across disciplines in LGBTQ health by assessing medical, dental, and nursing students’ perceptions of preparedness across three domains: comfort levels, attitudes, and formal training. Methods We developed a 12-item survey with an interprofessional panel of LGBTQ students from the schools of medicine, dental medicine, and nursing at a top-tier private university in the United States. Any student enrolled full time in any of the three schools were eligible to respond. We performed descriptive statistical analyses and examined patterns in responses using Kruskal-Wallis tests and an ordered logistic regression model. Results 1,010 students from the Schools of Medicine, Dental Medicine, and Nursing responded to the survey for an overall response rate of 43%. While 70–74% of all student respondents felt comfortable treating LGBTQ patients, fewer than 50% agreed that their formal training had prepared them to do so. Overall, 71–81% of students reported interest in receiving formal LGBTQ health education, though dental students were significantly less likely than medical students to report this interest (OR 0.53, p

Published

2018

7. Effective Treatment of SIVcpz-Induced Immunodeficiency in a Captive Western Chimpanzee

Author

Paul M. Sharp, Raven Jackson-Jewett, Edward P. Acosta, Thomas N. Denny, Gerald H. Learn, Frederic Bibollet-Ruche, Katharine J. Bar, Corrine S. Brown, Timothy Decker, Hannah J. Barbian, Yingying Li, Jeffrey D. Lifson, Edward F. Kreider, Beatrice H. Hahn, George M. Shaw, and Michael S. Saag

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Male, Pan troglodytes, antiretroviral therapy, Simian Acquired Immunodeficiency Syndrome, Short Report, Viremia, medicine.disease_cause, Virus, SIVcpz, 03 medical and health sciences, chemistry.chemical_compound, chimpanzees, Virology, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, medicine, Animals, Chimpanzees, Immunodeficiency, drug resistance, biology, Simian immunodeficiency virus, Viral Load, biology.organism_classification, medicine.disease, Resistance mutation, 3. Good health, CD4 Lymphocyte Count, Antiretroviral therapy, AIDS, Ape Diseases, 030104 developmental biology, Infectious Diseases, chemistry, Anti-Retroviral Agents, Drug resistance, Lentivirus, Immunology, Dolutegravir, Mutation, RNA, Viral, Simian Immunodeficiency Virus, lcsh:RC581-607, Viral load

Abstract

Background: Simian immunodefciency virus of chimpanzees (SIVcpz), the progenitor of human immunodefciency virus type 1 (HIV-1), is associated with increased mortality and AIDS-like immunopathology in wild-living chimpan‑ zees (Pan troglodytes). Surprisingly, however, similar fndings have not been reported for chimpanzees experimentally infected with SIVcpz in captivity, raising questions about the intrinsic pathogenicity of this lentivirus. Findings: Here, we report progressive immunodefciency and clinical disease in a captive western chimpanzee (P. t. verus) infected twenty years ago by intrarectal inoculation with an SIVcpz strain (ANT) from a wild-caught eastern chimpanzee (P. t. schweinfurthii). With sustained plasma viral loads of 105 to 106 RNA copies/ml for the past 15 years, this chimpanzee developed CD4+ T cell depletion (220 cells/μl), thrombocytopenia (90,000 platelets/μl), and persis‑ tent soft tissue infections refractory to antibacterial therapy. Combination antiretroviral therapy consisting of emtric‑ itabine (FTC), tenofovir disoproxil fumarate (TDF), and dolutegravir (DTG) decreased plasma viremia to undetectable levels (Conclusions: These data demonstrate that SIVcpz can cause immunodefciency and other hallmarks of AIDS in cap‑ tive chimpanzees, including P. t. verus apes that are not naturally infected with this virus. Moreover, SIVcpz-associated immunodefciency can be efectively treated with antiretroviral therapy, although sufciently high plasma concentra‑ tions must be maintained to prevent the emergence of drug resistance. These fndings extend a growing body of evidence documenting the immunopathogenicity of SIVcpz and suggest that experimentally infected chimpanzees may beneft from clinical monitoring and therapeutic intervention. Keywords: SIVcpz, Chimpanzees, Antiretroviral therapy, AIDS, Drug resistance

Published

2017

8. Antibody 10-1074 suppresses viremia in HIV-1-infected individuals

Author

Cecilia Unson-O’Brien, Daniela Weiland, Irina Shimeliovich, Michel C. Nussenzweig, Allison Settler, Edward F. Kreider, Maggi Witmer-Pack, Florian Klein, Kemal Eren, Christoph Wyen, Tim Kümmerle, Roy M. Gulick, Tibor Keler, Gerald H. Learn, Clara Lehmann, Thiago Y. Oliveira, Pamela J. Bjorkman, Caroline Ignacio, Hugo Mouquet, Yehuda Z. Cohen, Nico Pfeifer, Sarah J. Schlesinger, Michael S. Seaman, Till Schoofs, Gerd Fätkenheuer, Ben Murrell, Theodora K. Karagounis, Henning Gruell, Lilian Nogueira, Anthony P. West, Barry S. Zingman, Daniel Gillor, Marina Caskey, Beatrice H. Hahn, Rebeka Levin, Alexander. Robles, and Szilard Kiss

Subjects

Adult, Male, 0301 basic medicine, Glycan, medicine.drug_class, HIV Infections, Viremia, CHO Cells, HIV Antibodies, HIV Envelope Protein gp120, Monoclonal antibody, Article, General Biochemistry, Genetics and Molecular Biology, Virus, Epitope, law.invention, Young Adult, 03 medical and health sciences, Cricetulus, law, medicine, Animals, Humans, biology, env Gene Products, Human Immunodeficiency Virus, Antibodies, Monoclonal, General Medicine, Middle Aged, Viral Load, medicine.disease, Antibodies, Neutralizing, Virology, Peptide Fragments, Recombinant Proteins, CD4 Lymphocyte Count, 3. Good health, 030104 developmental biology, Immunoglobulin G, Immunology, HIV-1, Recombinant DNA, biology.protein, RNA, Viral, Female, Antibody, Viral load

Abstract

Florian Klein and colleagues report that treating viremic HIV-1-infected individuals with the broadly neutralizing antibody 10-1074 reduced virus levels in blood, but antibody-resistant virus did emerge. Monoclonal antibody 10-1074 targets the V3 glycan supersite on the HIV-1 envelope (Env) protein. It is among the most potent anti-HIV-1 neutralizing antibodies isolated so far. Here we report on its safety and activity in 33 individuals who received a single intravenous infusion of the antibody. 10-1074 was well tolerated and had a half-life of 24.0 d in participants without HIV-1 infection and 12.8 d in individuals with HIV-1 infection. Thirteen individuals with viremia received the highest dose of 30 mg/kg 10-1074. Eleven of these participants were 10-1074-sensitive and showed a rapid decline in viremia by a mean of 1.52 log10 copies/ml. Virologic analysis revealed the emergence of multiple independent 10-1074-resistant viruses in the first weeks after infusion. Emerging escape variants were generally resistant to the related V3-specific antibody PGT121, but remained sensitive to antibodies targeting nonoverlapping epitopes, such as the anti-CD4-binding-site antibodies 3BNC117 and VRC01. The results demonstrate the safety and activity of 10-1074 in humans and support the idea that antibodies targeting the V3 glycan supersite might be useful for the treatment and prevention of HIV-1 infection.

Published

2017

9. Staged induction of HIV-1 glycan–dependent broadly neutralizing antibodies

Author

S. Munir Alam, Mark K. Louder, Kevin Wiehe, Brendan W. Pier, Feng Gao, Barton F. Haynes, Kshitij Wagh, John R. Mascola, Morgan A. Gladden, Kwan-Ki Hwang, Peter T. Hraber, Ruijun Zhang, William E. Walkowicz, George M. Shaw, Stephen C. Harrison, Anthony Monroe, Beatrice H. Hahn, M. Anthony Moody, Hua-Xin Liao, Amit Kumar, Lynn Morris, Gift Kamanga, R. Ryan Meyerhoff, Kevin O. Saunders, Myron S. Cohen, Edward F. Kreider, Todd Bradley, Bette T. Korber, Robert T. Bailer, Mattia Bonsignori, John C. Kappes, Ashley M. Trama, Wilton B. Williams, Garnett Kelsoe, Daniela Fera, Shi-Mao Xia, Thomas B. Kepler, Claudia A. Jette, Samuel J. Danishefsky, Krisha McKee, Baptiste Aussedat, Melissa Cooper, and David C. Montefiori

Subjects

Male, 0301 basic medicine, Cytidine deaminase activity, Lineage (genetic), Somatic hypermutation, Crystallography, X-Ray, Article, Epitope, Virus, Affinity maturation, 03 medical and health sciences, Neutralization Tests, Polysaccharides, Humans, Neutralizing antibody, Phylogeny, biology, env Gene Products, Human Immunodeficiency Virus, General Medicine, Antibodies, Neutralizing, Virology, 030104 developmental biology, Mutation, HIV-1, biology.protein, Antibody, Protein Binding

Abstract

A preventive HIV-1 vaccine should induce HIV-1-specific broadly neutralizing antibodies (bnAbs). However, bnAbs generally require high levels of somatic hypermutation (SHM) to acquire breadth, and current vaccine strategies have not been successful in inducing bnAbs. Because bnAbs directed against a glycosylated site adjacent to the third variable loop (V3) of the HIV-1 envelope protein require limited SHM, the V3-glycan epitope is an attractive vaccine target. By studying the cooperation among multiple V3-glycan B cell lineages and their coevolution with autologous virus throughout 5 years of infection, we identify key events in the ontogeny of a V3-glycan bnAb. Two autologous neutralizing antibody lineages selected for virus escape mutations and consequently allowed initiation and affinity maturation of a V3-glycan bnAb lineage. The nucleotide substitution required to initiate the bnAb lineage occurred at a low-probability site for activation-induced cytidine deaminase activity. Cooperation of B cell lineages and an improbable mutation critical for bnAb activity defined the necessary events leading to breadth in this V3-glycan bnAb lineage. These findings may, in part, explain why initiation of V3-glycan bnAbs is rare, and suggest an immunization strategy for inducing similar V3-glycan bnAbs.

Published

2017

10. Effect of HIV Antibody VRC01 on Viral Rebound after Treatment Interruption

Author

KaSaundra Oden, John R. Mascola, Michael Messer, Bernadette Jarocki, Barney S. Graham, James A. Hoxie, Anthony S. Fauci, Sijy O'Dell, Rebecca M. Lynch, Katharine J. Bar, Jana Blazkova, Nicole A. Doria-Rose, Mary E. Petrone, Benjamin Scheinfeld, Randall Tressler, Richard Kwan, Edward F. Kreider, Edmund V. Capparelli, Linda Harrison, Edgar T. Overton, Gerald H. Learn, Richard A. Koup, Michael C. Sneller, D. Brenda Salantes, Michael A. Proschan, Pablo Tebas, Katherine E Clarridge, Catherine Seamon, Nancy B Tustin, Robert T. Bailer, J. Shawn Justement, Julie E. Ledgerwood, Eric W. Refsland, Susan Moir, Tae-Wook Chun, Andrea Shiakolas, Mark Bardsley, and Patrick J Madden

Subjects

0301 basic medicine, Adult, Male, Viremia, HIV Infections, HIV Antibodies, Article, 03 medical and health sciences, 0302 clinical medicine, Acquired immunodeficiency syndrome (AIDS), medicine, Humans, 030212 general & internal medicine, Adverse effect, Phylogeny, Aged, biology, business.industry, env Gene Products, Human Immunodeficiency Virus, Antibodies, Monoclonal, HIV, Historically Controlled Study, General Medicine, Middle Aged, Viral Load, medicine.disease, Antibodies, Neutralizing, Discontinuation, Clinical trial, 030104 developmental biology, Immunization, Immunology, HIV-1, biology.protein, RNA, Viral, Female, Antibody, business, Viral load, Broadly Neutralizing Antibodies

Abstract

The discovery of potent and broadly neutralizing antibodies (bNAbs) against human immunodeficiency virus (HIV) has made passive immunization a potential strategy for the prevention and treatment of HIV infection. We sought to determine whether passive administration of VRC01, a bNAb targeting the HIV CD4-binding site, can safely prevent or delay plasma viral rebound after the discontinuation of antiretroviral therapy (ART).We conducted two open-label trials (AIDS Clinical Trials Group [ACTG] A5340 and National Institutes of Health [NIH] 15-I-0140) of the safety, side-effect profile, pharmacokinetic properties, and antiviral activity of VRC01 in persons with HIV infection who were undergoing interruption of ART.A total of 24 participants were enrolled, and one serious alcohol-related adverse event occurred. Viral rebound occurred despite plasma VRC01 concentrations greater than 50 μg per milliliter. The median time to rebound was 4 weeks in the A5340 trial and 5.6 weeks in the NIH trial. Study participants were more likely than historical controls to have viral suppression at week 4 (38% vs. 13%, P=0.04 by a two-sided Fisher's exact test in the A5340 trial; and 80% vs. 13%, P0.001 by a two-sided Fisher's exact test in the NIH trial) but the difference was not significant at week 8. Analyses of virus populations before ART as well as before and after ART interruption showed that VRC01 exerted pressure on rebounding virus, resulting in restriction of recrudescent viruses and selection for preexisting and emerging antibody neutralization-resistant virus.VRC01 slightly delayed plasma viral rebound in the trial participants, as compared with historical controls, but it did not maintain viral suppression by week 8. In the small number of participants enrolled in these trials, no safety concerns were identified with passive immunization with a single bNAb (VRC01). (Funded by the National Institute of Allergy and Infectious Diseases and others; ACTG A5340 and NIH 15-I-0140 ClinicalTrials.gov numbers, NCT02463227 and NCT02471326 .).

Published

2016

11. Paired quantitative and qualitative assessment of the replication-competent HIV-1 reservoir and comparison with integrated proviral DNA

Author

Christy L. Lavine, Michel C. Nussenzweig, Lillian B. Cohn, Allison Settler, Yehuda Z. Cohen, Marina Caskey, Joshua A. Horwitz, Thiago Y. Oliveira, Michael S. Seaman, Beatrice H. Hahn, Mila Jankovic, Gerald H. Learn, Arup K. Chakraborty, John P. Barton, Edward F. Kreider, and Julio C. C. Lorenzi

Subjects

0301 basic medicine, reservoir, Sequence analysis, viruses, Human immunodeficiency virus (HIV), Clone (cell biology), Proviral dna, Biology, medicine.disease_cause, Corrections, Virus, Defective virus, 03 medical and health sciences, medicine, 2.2 Factors relating to the physical environment, Aetiology, Genetics, replication-competent, Multidisciplinary, HIV, Leukapheresis, Virology, Antiretroviral therapy, culture, Infectious Diseases, Good Health and Well Being, 030104 developmental biology, method, HIV/AIDS, Infection

Abstract

HIV-1-infected individuals harbor a latent reservoir of infected CD4+ T cells that is not eradicated by antiretroviral therapy (ART). This reservoir presents the greatest barrier to an HIV-1 cure and has remained difficult to characterize, in part, because the vast majority of integrated sequences are defective and incapable of reactivation. To characterize the replication-competent reservoir, we have combined two techniques, quantitative viral outgrowth and qualitative sequence analysis of clonal outgrowth viruses. Leukapheresis samples from four fully ART-suppressed, chronically infected individuals were assayed at two time points separated by a 4- to 6-mo interval. Overall, 54% of the viruses emerging from the latent reservoir showed gp160 env sequences that were identical to at least one other virus. Moreover, 43% of the env sequences from viruses emerging from the reservoir were part of identical groups at the two time points. Groups of identical expanded sequences made up 54% of proviral DNA, and, as might be expected, the sequences of replication-competent viruses in the active reservoir showed limited overlap with integrated proviral DNA, most of which is known to represent defective viruses. Finally, there was an inverse correlation between proviral DNA clone size and the probability of reactivation, suggesting that replication-competent viruses are less likely to be found among highly expanded provirus-containing cell clones.

Published

2016

12. HIV-1 antibody 3BNC117 suppresses viral rebound in humans during treatment interruption

Author

Florian Klein, Michel C. Nussenzweig, Nico Pfeifer, Yehuda Z. Cohen, Anthony P. West, Irina Shimeliovich, Marina Caskey, Tibor Keler, Gerald H. Learn, Allison Settler, Lilian Nogueira, Barry S. Zingman, Yotam Bar-On, Pamela J. Bjorkman, Sonya Hadrigan, Ching-Lan Lu, Thiago Y. Oliveira, Thomas Hawthorne, Anna Feldmann, Johannes F. Scheid, Joshua A. Horwitz, Malte Braunschweig, Boris Juelg, Bruce D. Walker, Maggi Witmer-Pack, Edward F. Kreider, Roshni Patel, Julio C. C. Lorenzi, Beatrice H. Hahn, Sarah J. Schlesinger, Michael S. Seaman, Leah A. Burke, and Roy M. Gulick

Subjects

0301 basic medicine, Adult, Male, Disease reservoir, Time Factors, Adolescent, Anti-HIV Agents, HIV Infections, HIV Antibodies, Antibodies, Monoclonal, Humanized, Virus, Article, Drug Administration Schedule, HIV Envelope Protein gp160, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Proviruses, Medicine, Humans, Tissue Distribution, Young adult, Neutralizing antibody, Aged, Disease Reservoirs, Multidisciplinary, Binding Sites, biology, business.industry, Historically Controlled Study, Provirus, Middle Aged, Viral Load, Virology, Antibodies, Neutralizing, 030104 developmental biology, 030220 oncology & carcinogenesis, Immunology, Monoclonal, CD4 Antigens, biology.protein, HIV-1, Female, Antibody, business, Viral load, Broadly Neutralizing Antibodies

Abstract

Interruption of combination antiretroviral therapy in HIV-1-infected individuals leads to rapid viral rebound. Here we report the results of a phase IIa open label clinical trial evaluating 3BNC117,a broad and potent neutralizing antibody against the CD4 binding site of the HIV-1 Env protein, during analytical treatment interruption in 13 HIV-1-infected individuals. Participants with 3BNC117-sensitive virus outgrowth cultures were enrolled. Results show that two or four 30 mg kg(-1) 3BNC117 infusions,separated by 3 or 2 weeks, respectively, are generally well tolerated.Infusions are associated with a delay in viral rebound of 5-9 weeks after two infusions, and up to 19 weeks after four infusions, or an average of 6.7 and 9.9 weeks, respectively, compared with 2.6 weeks for historical controls (P < 0.00001). Rebound viruses arise predominantly from a single provirus. In most individuals,emerging viruses show increased resistance, indicating escape.However, 30% of participants remained suppressed until antibody concentrations waned below 20 μg ml(-1), and the viruses emerging in all but one of these individuals showed no apparent resistance to 3BCN117, suggesting failure to escape over a period of 9-19 weeks.We conclude that the administration of 3BNC117 exerts strong selective pressure on HIV-1 emerging from latent reservoirs during analytical treatment interruption in humans.

Published

2016

13. HIV-1 therapy with monoclonal antibody 3BNC117 elicits host immune responses against HIV-1

Author

Lilian Nogueira, Nico Pfeifer, Julie Czartoski, Beatrice H. Hahn, M. Juliana McElrath, Michel C. Nussenzweig, Marina Caskey, Florian Klein, Sarah J. Schlesinger, Malte Braunschweig, Michael S. Seaman, Edward F. Kreider, Thiago Y. Oliveira, Gerald H. Learn, Pamela J. Bjorkman, Anthony P. West, Till Schoofs, Erica H. Parrish, Julio C. C. Lorenzi, and Anna Feldmann

Subjects

0301 basic medicine, Adult, Male, medicine.medical_treatment, Viremia, HIV Infections, HIV Antibodies, Antibodies, Monoclonal, Humanized, Article, 03 medical and health sciences, Young Adult, Immune system, Viral envelope, Immunity, medicine, Humans, Amino Acid Sequence, Neutralizing antibody, Phylogeny, Multidisciplinary, biology, Immunization, Passive, Antibodies, Monoclonal, Immunotherapy, Middle Aged, medicine.disease, Virology, Antibodies, Neutralizing, 3. Good health, Immunity, Humoral, 030104 developmental biology, Humoral immunity, Immunology, Antibody Formation, biology.protein, HIV-1, Female, Antibody, Broadly Neutralizing Antibodies

Abstract

3BNC117 is a broad and potent anti-HIV-1 neutralizing antibody that targets the CD4 binding site on the viral envelope spike. When administered passively, this antibody can prevent infection in animal models and suppress viremia in HIV-1-infected individuals. Here we report that HIV-1 immunotherapy with a single injection of 3BNC117 impacts host antibody responses in viremic subjects. In comparison to untreated controls that showed little change in their neutralizing activity over a six-month period, 3BNC117 infusion significantly improved neutralizing responses to heterologous tier 2 viruses in nearly all study participants. We conclude that 3BNC117-mediated immunotherapy enhances host humoral immunity to HIV-1.

Published

2016

14. Completeness of HIV-1 Envelope Glycan Shield at Transmission Determines Neutralization Breadth

Author

Peter D. Kwong, Jamie Wandzilak, Barton F. Haynes, Reda Rawi, Peter T. Hraber, Kshitij Wagh, Pierre Pellegrino, Gerald H. Learn, Ian Williams, Edward F. Kreider, Julie Overbaugh, Feng Gao, Lindsey Gillis, Gwo-Yu Chuang, Bette T. Korber, Timothy Decker, Michael S. Seaman, Hannah J. Barbian, Yingying Li, George M. Shaw, Beatrice H. Hahn, Andrew G. Smith, Elena E. Giorgi, Fangping Cai, Persephone Borrow, and Marcos V. P. Gondim

Subjects

0301 basic medicine, Models, Molecular, Glycan, Biology, Hiv 1 envelope, General Biochemistry, Genetics and Molecular Biology, Neutralization, Article, 03 medical and health sciences, Neutralization Tests, Polysaccharides, Humans, lcsh:QH301-705.5, Conserved Sequence, env Gene Products, Human Immunodeficiency Virus, virus diseases, Computational Biology, Virology, Antibodies, Neutralizing, 3. Good health, carbohydrates (lipids), Kinetics, 030104 developmental biology, HEK293 Cells, lcsh:Biology (General), biology.protein, HIV-1

Abstract

SUMMARY Densely arranged N-linked glycans shield the HIV-1 envelope (Env) trimer from antibody recognition. Strain-specific breaches in this shield (glycan holes) can be targets of vaccine-induced neutralizing antibodies that lack breadth. To understand the interplay between glycan holes and neutralization breadth in HIV-1 infection, we developed a sequence-and structure-based approach to identify glycan holes for individual Env sequences that are shielded in most M-group viruses. Applying this approach to 12 longitudinally followed individuals, we found that transmitted viruses with more intact glycan shields correlated with development of greater neutralization breadth. Within 2 years, glycan acquisition filled most glycan holes present at transmission, indicating escape from hole-targeting neutralizing antibodies. Glycan hole filling generally preceded the time to first detectable breadth, although time intervals varied across hosts. Thus, completely glycan-shielded viruses were associated with accelerated neutralization breadth development, suggesting that Env immunogens with intact glycan shields may be preferred components of AIDS vaccines., In Brief Wagh et al. show that transmitted viruses with more intact glycan shields are correlated with development of neutralization breadth in HIV-1-infected individuals. This is consistent with previous findings that glycan holes in Env immunogens are targeted by strain-specific neutralizing responses, and suggests that immunogens with intact glycan Shields may be advantageous., Graphical Abstract

Published

2018

15. Longitudinal Antigenic Sequences and Sites from Intra-Host Evolution (LASSIE) Identifies Immune-Selected HIV Variants

Author

Yingying Li, Mattia Bonsignori, M. A. Moody, Bette T. Korber, Peter T. Hraber, Feng Gao, Gerald H. Learn, S.M. Alam, Barton F. Haynes, Alan Lapedes, Beatrice H. Hahn, Kshitij Wagh, George M. Shaw, Hua-Xin Liao, Sandrasegaram Gnanakaran, Edward F. Kreider, Elena E. Giorgi, Tanmoy Bhattacharya, and David C. Montefiori

Subjects

immunogen design, lcsh:QR1-502, envelope glycoprotein, selection, HIV Infections, Viral quasispecies, Biology, Quantitative Biology - Quantitative Methods, lcsh:Microbiology, DNA sequencing, Epitope, Virus, Article, human immunodeficiency virus type 1, Antigen, Virology, vaccine, Genetic variation, neutralizing antibodies, coevolution, immune escape, quasispecies, antigenic swarm, Humans, Longitudinal Studies, Selection, Genetic, Quantitative Biology - Populations and Evolution, Antigens, Viral, Quantitative Methods (q-bio.QM), Immune Evasion, Genetics, Phylogenetic tree, Populations and Evolution (q-bio.PE), Genetic Variation, HIV, 3. Good health, Infectious Diseases, FOS: Biological sciences, biology.protein, Antibody

Abstract

Within-host genetic sequencing from samples collected over time provides a dynamic view of how viruses evade host immunity. Immune-driven mutations might stimulate neutralization breadth by selecting antibodies adapted to cycles of immune escape that generate within-subject epitope diversity. Comprehensive identification of immune-escape mutations is experimentally and computationally challenging. With current technology, many more viral sequences can readily be obtained than can be tested for binding and neutralization, making down-selection necessary. Typically, this is done manually, by picking variants that represent different time-points and branches on a phylogenetic tree. Such strategies are likely to miss many relevant mutations and combinations of mutations, and to be redundant for other mutations. Longitudinal Antigenic Sequences and Sites from Intrahost Evolution (LASSIE) uses transmitted-founder loss to identify virus "hot-spots" under putative immune selection and chooses sequences that represent recurrent mutations in selected sites. LASSIE favors earliest sequences in which mutations arise. With well-characterized longitudinal Env sequences, we confirmed selected sites were concentrated in antibody contacts and selected sequences represented diverse antigenic phenotypes. Practical applications include rapidly identifying immune targets under selective pressure within a subject, selecting minimal sets of reagents for immunological assays that characterize evolving antibody responses, and for immunogens in polyvalent "cocktail" vaccines., 73 pages, 10 figures, 8 supplemental figures; 18 full-resolution figures appear at the end of the manuscript. Presented at 22nd International Workshop on HIV Dynamics and Evolution, Budapest, May 2015

Published

2015

16. A Naturally Occurring rev1-vpu Fusion Gene Does Not Confer a Fitness Advantage to HIV-1

Author

Beatrice H. Hahn, Daniel Sauter, Edward F. Kreider, Lan-Hui Lee, Gerald H. Learn, Simon Langer, Kristina Hopfensperger, and Shilpa S. Iyer

Subjects

Gene Expression Regulation, Viral, animal diseases, viruses, Human Immunodeficiency Virus Proteins, lcsh:Medicine, Viral quasispecies, Biology, Fusion gene, 03 medical and health sciences, Exon, Humans, Viral Regulatory and Accessory Proteins, lcsh:Science, Gene, 030304 developmental biology, Genetics, Regulation of gene expression, 0303 health sciences, Multidisciplinary, 030302 biochemistry & molecular biology, lcsh:R, virus diseases, rev Gene Products, Human Immunodeficiency Virus, biochemical phenomena, metabolism, and nutrition, Fusion protein, Virology, 3. Good health, HEK293 Cells, Viral replication, Tetherin, HIV-1, RNA, Viral, lcsh:Q, Gene Fusion, Research Article

Abstract

Background Pandemic strains of HIV-1 (group M) encode a total of nine structural (gag, pol, env), regulatory (rev, tat) and accessory (vif, vpr, vpu, nef) genes. However, some subtype A and C viruses exhibit an unusual gene arrangement in which the first exon of rev (rev1) and the vpu gene are placed in the same open reading frame. Although this rev1-vpu gene fusion is present in a considerable fraction of HIV-1 strains, its functional significance is unknown. Results Examining infectious molecular clones (IMCs) of HIV-1 that encode the rev1-vpu polymorphism, we show that a fusion protein is expressed in infected cells. Due to the splicing pattern of viral mRNA, however, these same IMCs also express a regular Vpu protein, which is produced at much higher levels. To investigate the function of the fusion gene, we characterized isogenic IMC pairs differing only in their ability to express a Rev1-Vpu protein. Analysis in transfected HEK293T and infected CD4+ T cells showed that all of these viruses were equally active in known Vpu functions, such as down-modulation of CD4 or counteraction of tetherin. Furthermore, the polymorphism did not affect Vpu-mediated inhibition of NF-кB activation or Rev-dependent nuclear export of incompletely spliced viral mRNAs. There was also no evidence for enhanced replication of Rev1-Vpu expressing viruses in primary PBMCs or ex vivo infected human lymphoid tissues. Finally, the frequency of HIV-1 quasispecies members that encoded a rev1-vpu fusion gene did not change in HIV-1 infected individuals over time. Conclusions Expression of a rev1-vpu fusion gene does not affect regular Rev and Vpu functions or alter HIV-1 replication in primary target cells. Since there is no evidence for increased replication fitness of rev1-vpu encoding viruses, this polymorphism likely emerged in the context of other mutations within and/or outside the rev1-vpu intergenic region, and may have a neutral phenotype.

Published

2015

17. Comprehensive Analysis of LANA Interacting Proteins Essential for Viral Genome Tethering and Persistence

Author

Qiliang Cai, Subhash C. Verma, Jie Lu, Erle S. Robertson, and Edward F. Kreider

Subjects

viruses, Green Fluorescent Proteins, lcsh:Medicine, Genome, Viral, DNA-binding protein, Histones, 03 medical and health sciences, Histone H1, HMGB Proteins, Lymphoma, Primary Effusion, Two-Hybrid System Techniques, Histone H2A, medicine, Fluorescence Resonance Energy Transfer, Nucleosome, Deoxyribonuclease I, Humans, Immunoprecipitation, Micrococcal Nuclease, lcsh:Science, Antigens, Viral, 030304 developmental biology, Cell Proliferation, Glutathione Transferase, 0303 health sciences, Multidisciplinary, Alanine, biology, Cell Death, lcsh:R, 030302 biochemistry & molecular biology, Lentivirus, virus diseases, Nuclear Proteins, medicine.disease, Molecular biology, Chromatin, 3. Good health, Histone, High-mobility group, Herpesvirus 8, Human, biology.protein, lcsh:Q, Primary effusion lymphoma, Research Article, Protein Binding

Abstract

Kaposi's sarcoma associated herpesvirus is tightly linked to multiple human malignancies including Kaposi's sarcoma (KS), Primary Effusion Lymphoma (PEL) and Multicentric Castleman's Disease (MCD). KSHV like other herpesviruses establishes life-long latency in the infected host by persisting as chromatin and tethering to host chromatin through the virally encoded protein Latency Associated Nuclear Antigen (LANA). LANA, a multifunctional protein, is capable of binding to a large number of cellular proteins responsible for transcriptional regulation of various cellular and viral pathways involved in blocking cell death and promoting cell proliferation. This leads to enhanced cell division and replication of the viral genome, which segregates faithfully in the dividing tumor cells. The mechanism of genome segregation is well known and the binding of LANA to nucleosomal proteins, throughout the cell cycle, suggests that these interactions play an important role in efficient segregation. Various biochemical methods have identified a large number of LANA binding proteins, including histone H2A/H2B, histone H1, MeCP2, DEK, CENP-F, NuMA, Bub1, HP-1, and Brd4. These nucleosomal proteins may have various functions in tethering of the viral genome during specific phases of the viral life cycle. Therefore, we performed a comprehensive analysis of their interaction with LANA using a number of different assays. We show that LANA binds to core nucleosomal histones and also associates with other host chromatin proteins including histone H1 and high mobility group proteins (HMGs). We used various biochemical assays including co-immunoprecipitation and in-vivo localization by split GFP and fluorescence resonance energy transfer (FRET) to demonstrate their association.

Published

2013

18. A Naturally Occurring rev1-vpu Fusion Gene Does Not Confer a Fitness Advantage to HIV-1.

Author

Simon M Langer, Kristina Hopfensperger, Shilpa S Iyer, Edward F Kreider, Gerald H Learn, Lan-Hui Lee, Beatrice H Hahn, and Daniel Sauter

Subjects

Medicine, Science

Abstract

Pandemic strains of HIV-1 (group M) encode a total of nine structural (gag, pol, env), regulatory (rev, tat) and accessory (vif, vpr, vpu, nef) genes. However, some subtype A and C viruses exhibit an unusual gene arrangement in which the first exon of rev (rev1) and the vpu gene are placed in the same open reading frame. Although this rev1-vpu gene fusion is present in a considerable fraction of HIV-1 strains, its functional significance is unknown.Examining infectious molecular clones (IMCs) of HIV-1 that encode the rev1-vpu polymorphism, we show that a fusion protein is expressed in infected cells. Due to the splicing pattern of viral mRNA, however, these same IMCs also express a regular Vpu protein, which is produced at much higher levels. To investigate the function of the fusion gene, we characterized isogenic IMC pairs differing only in their ability to express a Rev1-Vpu protein. Analysis in transfected HEK293T and infected CD4+ T cells showed that all of these viruses were equally active in known Vpu functions, such as down-modulation of CD4 or counteraction of tetherin. Furthermore, the polymorphism did not affect Vpu-mediated inhibition of NF-кB activation or Rev-dependent nuclear export of incompletely spliced viral mRNAs. There was also no evidence for enhanced replication of Rev1-Vpu expressing viruses in primary PBMCs or ex vivo infected human lymphoid tissues. Finally, the frequency of HIV-1 quasispecies members that encoded a rev1-vpu fusion gene did not change in HIV-1 infected individuals over time.Expression of a rev1-vpu fusion gene does not affect regular Rev and Vpu functions or alter HIV-1 replication in primary target cells. Since there is no evidence for increased replication fitness of rev1-vpu encoding viruses, this polymorphism likely emerged in the context of other mutations within and/or outside the rev1-vpu intergenic region, and may have a neutral phenotype.

Published

2015