Your search keyword '"Zabrina L. Brumme"' showing total 309 results

201. No evidence for selection of HIV-1 with enhanced Gag-Protease or Nef function among breakthrough infections in the CAPRISA 004 tenofovir microbicide trial

Author

Sarah Goodier, Eric Martin, Xiaomei T. Kuang, Quarraisha Abdool Karim, Zabrina L. Brumme, Saleha Omarjee, Vivek Naranbhai, Salim S. Abdool Karim, Philip Mwimanzi, Nonkululeko. Ndabambi, Denis Chopera, Mark A. Brockman, Carolyn Williamson, Thumbi Ndung'u, Jaclyn K. Mann, Division of Virology, and Faculty of Health Sciences

Subjects

Anti-HIV Agents, medicine.medical_treatment, viruses, Natural selection, Organophosphonates, T cells, lcsh:Medicine, HIV Infections, Biology, Virus Replication, gag Gene Products, Human Immunodeficiency Virus, 03 medical and health sciences, Microbicide, CAPRISA 004, medicine, Viral replication, Humans, nef Gene Products, Human Immunodeficiency Virus, Tenofovir, lcsh:Science, Phylogeny, Selection (genetic algorithm), 030304 developmental biology, Clinical Trials as Topic, 0303 health sciences, Multidisciplinary, Protease, 030306 microbiology, Transmission (medicine), Prophylaxis, Adenine, lcsh:R, Sequence analysis, virus diseases, Sequence Analysis, DNA, Virology, 3. Good health, Microbicides, Microbicides for sexually transmitted diseases, Immunology, Vaginal Creams, Foams, and Jellies, HIV-1, Female, lcsh:Q, Function (biology), Research Article, Cloning

Abstract

BACKGROUND: Use of antiretroviral-based microbicides for HIV-1 prophylaxis could introduce a transmission barrier that inadvertently facilitates the selection of fitter viral variants among incident infections. To investigate this, we assessed the in vitro function of gag-protease and nef sequences from participants who acquired HIV-1 during the CAPRISA 004 1% tenofovir microbicide gel trial. Methods and RESULTS: We isolated the earliest available gag-protease and nef gene sequences from 83 individuals and examined their in vitro function using recombinant viral replication capacity assays and surface protein downregulation assays, respectively. No major phylogenetic clustering and no significant differences in gag-protease or nef function were observed in participants who received tenofovir gel versus placebo gel prophylaxis. CONCLUSION: Results indicate that the partial protective effects of 1% tenofovir gel use in the CAPRISA 004 trial were not offset by selection of transmitted/early HIV-1 variants with enhanced Gag-Protease or Nef fitness.

Published

2013

202. Correlates of Protective Cellular Immunity Revealed by Analysis of Population-Level Immune Escape Pathways in HIV-1

Author

Mark A. Brockman, Sharon A. Riddler, P. Richard Harrigan, Chanson J. Brumme, Anh Q. Le, Richard Apps, Simon Mallal, George W. Nelson, Eric Martin, Charles E. DeZiel, Zabrina L. Brumme, Jonathan M. Carlson, David J.H.F. Knapp, Celia K. S. Chui, Mina John, Jennifer Listgarten, Laura A. Cotton, Richard Haubrich, Mary Carrington, Nico Pfeifer, and David Heckerman

Subjects

Genetics, Cellular immunity, Immunity, Cellular, Immunogenicity, Immunology, Human leukocyte antigen, Biology, Microbiology, Epitope, Histocompatibility, CTL, Epitopes, Immune system, HLA Antigens, Virology, Insect Science, HIV-1, Pathogenesis and Immunity, Humans, Allele, Alleles, Immune Evasion

Abstract

HLA class I-associated polymorphisms identified at the population level mark viral sites under immune pressure by individual HLA alleles. As such, analysis of their distribution, frequency, location, statistical strength, sequence conservation, and other properties offers a unique perspective from which to identify correlates of protective cellular immunity. We analyzed HLA-associated HIV-1 subtype B polymorphisms in 1,888 treatment-naïve, chronically infected individuals using phylogenetically informed methods and identified characteristics of HLA-associated immune pressures that differentiate protective and nonprotective alleles. Over 2,100 HLA-associated HIV-1 polymorphisms were identified, approximately one-third of which occurred inside or within 3 residues of an optimally defined cytotoxic T-lymphocyte (CTL) epitope. Differential CTL escape patterns between closely related HLA alleles were common and increased with greater evolutionary distance between allele group members. Among 9-mer epitopes, mutations at HLA-specific anchor residues represented the most frequently detected escape type: these occurred nearly 2-fold more frequently than expected by chance and were computationally predicted to reduce peptide-HLA binding nearly 10-fold on average. Characteristics associated with protective HLA alleles (defined using hazard ratios for progression to AIDS from natural history cohorts) included the potential to mount broad immune selection pressures across all HIV-1 proteins except Nef, the tendency to drive multisite and/or anchor residue escape mutations within known CTL epitopes, and the ability to strongly select mutations in conserved regions within HIV's structural and functional proteins. Thus, the factors defining protective cellular immune responses may be more complex than simply targeting conserved viral regions. The results provide new information to guide vaccine design and immunogenicity studies.

Published

2012

203. Significant reductions in Gag-protease-mediated HIV-1 replication capacity during the course of the epidemic in Japan

Author

Ai Kawana-Tachikawa, Mark A. Brockman, Aikichi Iwamoto, Zabrina L. Brumme, Michiko Koga, Tadashi Kikuchi, Toshiyuki Miura, Tomohiko Koibuchi, Noriaki Hosoya, Takeshi Fujii, Jonathan M. Carlson, David Heckerman, Shigeru Nomura, and Hitomi Nakamura

Subjects

Adult, Male, Adolescent, T cell, medicine.medical_treatment, T-Lymphocytes, Immunology, Green Fluorescent Proteins, Molecular Sequence Data, HIV Infections, Biology, Virus Replication, Microbiology, gag Gene Products, Human Immunodeficiency Virus, Cell Line, Young Adult, HIV Protease, Japan, Genes, Reporter, Virology, medicine, Humans, Aged, Genetics, Protease, Molecular epidemiology, Host (biology), Strain (biology), Sequence Analysis, DNA, Middle Aged, medicine.anatomical_structure, Genetic distance, Viral replication, Cell culture, Insect Science, HIV-1, Pathogenesis and Immunity, Female

Abstract

Human immunodeficiency virus type 1 (HIV-1) evolves rapidly in response to host immune selection pressures. As a result, the functional properties of HIV-1 isolates from earlier in the epidemic may differ from those of isolates from later stages. However, few studies have investigated alterations in viral replication capacity (RC) over the epidemic. In the present study, we compare Gag-Protease-associated RC between early and late isolates in Japan (1994 to 2009). HIV-1 subtype B sequences from 156 antiretroviral-naïve Japanese with chronic asymptomatic infection were used to construct a chimeric NL4-3 strain encoding plasma-derived gag-protease . Viral replication capacity was examined by infecting a long terminal repeat-driven green fluorescent protein-reporter T cell line. We observed a reduction in the RC of chimeric NL4-3 over the epidemic, which remained significant after adjusting for the CD4 + T cell count and plasma virus load. The same outcome was seen when limiting the analysis to a single large cluster of related sequences, indicating that our results are not due to shifts in the molecular epidemiology of the epidemic in Japan. Moreover, the change in RC was independent of genetic distance between patient-derived sequences and wild-type NL4-3, thus ruling out potential temporal bias due to genetic similarity between patient and historic viral backbone sequences. Collectively, these data indicate that Gag-Protease-associated HIV-1 replication capacity has decreased over the epidemic in Japan. Larger studies from multiple geographical regions will be required to confirm this phenomenon.

Published

2012

204. HLA-associated viral polymorphism in chronically HIV-1-infected Japanese cohort: analysis of four-digit HLA allele level

Author

Takayuki Chikata, Jonathan M. Carlson, Michihiro Hashimoto, Simon Mallal, Zabrina L. Brumme, Hiroyuki Gatanaga, Masafumi Takiguchi, Shinichi Oka, Mohamed Ali Borghan, Yoshiko Tamura, Mina John, and Takuya Naruto

Subjects

Genetics, biology, viruses, Human leukocyte antigen, Virus, Infectious Diseases, Immune system, Polymorphism (computer science), Virology, Poster Presentation, Immunology, biology.protein, Antibody, Allele, Clade, Cohort study

Abstract

It is assumed that the difference of HLA class I distribution among ethnic populations influences HIV evolution because HLA-restricted immune pressure selects escape mutations. Approximately 50% of HLA class I alleles are shared between Japanese and Caucasians. The analysis of HLA-associated polymorphism (HLA-AP) in both Japanese and Caucasian infected with clade B virus is expected to clarify the difference of HIV-1 evolution between both populations.

Published

2012

205. Modulation of HIV reservoirs by host HLA: bridging the gap between vaccine and cure

Author

Zabrina L. Brumme, Mark A. Brockman, and Denis Chopera

Subjects

AIDS Vaccines, Cellular immunity, Human immunodeficiency virus (HIV), virus diseases, HIV Infections, Human leukocyte antigen, Biology, medicine.disease_cause, Virology, Virus Latency, Immune system, HLA Antigens, Immunology, medicine, HIV-1, Animals, Humans, HIV vaccine

Abstract

Latent HIV reservoirs are the greatest challenge facing an HIV cure. Here, we review recent evidence supporting an important role for the host immune response, in particular HLA class I-restricted CD8+ T lymphocytes, in modulating HIV reservoirs during natural infection. These observations indicate that factors governing immune-mediated control of HIV may also contribute to the clearance of viral reservoirs. As such, critical gaps in our understanding of HIV immunology hinder efforts to develop both an effective HIV vaccine as well as novel therapies that may lead to a cure. The importance of elucidating correlates of protective cellular immunity should be recognized during research to develop and test potential HIV elimination strategies.

Published

2012

206. T cell receptor clonotypes modulate the protective effect of HLA class I alleles in HIV-1 infection

Author

Xu G. Yu, Zabrina L. Brumme, Huabiao Chen, Thai Duong Hong Cung, Daniel C. Douek, Toshiyuki Miura, Alicja Piechocka-Trocha, Arne Schneidewind, Sam Darko, Justin Fang, Todd M. Allen, Jennifer Sela, Florencia Pereyra, Ildiko Toth, Bruce D. Walker, Lindsay C. Porter, Zaza M. Ndhlovu, Dongfang Liu, Daniel Kaufmann, Mark A. Brockman, and Kevin Cesa

Subjects

Immunology, Receptors, Antigen, T-Cell, Epitopes, T-Lymphocyte, HIV Infections, Human leukocyte antigen, CD8-Positive T-Lymphocytes, Virus Replication, gag Gene Products, Human Immunodeficiency Virus, Epitope, Article, HIV Long-Term Survivors, Antigen, HLA-B Antigens, Humans, Immunology and Allergy, Cells, Cultured, HLA-B27 Antigen, biology, Perforin, T-cell receptor, Virology, Viral replication, HIV-1, biology.protein, CD8

Abstract

The human leukocyte antigens HLA-B27 and HLA-B57 are associated with protection against progression of disease that results from infection with human immunodeficiency virus type 1 (HIV-1), yet most people with alleles encoding HLA-B27 and HLA-B57 are unable to control HIV-1. Here we found that HLA-B27-restricted CD8(+) T cells in people able to control infection with HIV-1 (controllers) and those who progress to disease after infection with HIV-1 (progressors) differed in their ability to inhibit viral replication through targeting of the immunodominant epitope of group-associated antigen (Gag) of HIV-1. This was associated with distinct T cell antigen receptor (TCR) clonotypes, characterized by superior control of HIV-1 replication in vitro, greater cross-reactivity to epitope variants and enhanced loading and delivery of perforin. We also observed clonotype-specific differences in antiviral efficacy for an immunodominant HLA-B57-restricted response in controllers and progressors. Thus, the efficacy of such so-called 'protective alleles' is modulated by specific TCR clonotypes selected during natural infection, which provides a functional explanation for divergent HIV-1 outcomes.

Published

2012

207. Aminopeptidase substrate preference affects HIV epitope presentation and predicts immune escape patterns in HIV-infected individuals

Author

Zabrina L. Brumme, Huabiao Chen, Sasha B. Godfrey, Mariko Shimada, Eric Martin, Chanson J. Brumme, Jonathan M. Carlson, Bruce D. Walker, Sylvie Le Gall, Shao Chong Zhang, Paul Liebesny, Shirley Locastro, Jennifer Fricke, Daniel G. Kavanagh, Oluwatobi Awele Ogbechie, and Nicole Y. Lai

Subjects

Immunology, Antigen presentation, Human Immunodeficiency Virus Proteins, Epitopes, T-Lymphocyte, HIV Infections, Cell Separation, Lymphocyte Activation, Aminopeptidase, Aminopeptidases, Epitope, Article, Immune system, MHC class I, Immunology and Allergy, Humans, Immune Evasion, Antigen Presentation, Linear epitope, biology, Histocompatibility Antigens Class I, Flow Cytometry, Virology, CTL, Viral evolution, Mutation, biology.protein

Abstract

Viruses evade immune detection partly through immune-associated mutations. Analyses of HIV sequences derived from infected individuals have identified numerous examples of HLA-associated mutations within or adjacent to T cell epitopes, but the potential impact of most mutations on epitope production and presentation remains unclear. The multistep breakdown of proteins into epitopes includes trimming of N-extended peptides into epitopes by aminopeptidases before loading onto MHC class I molecules. Definition of sequence signatures that modulate epitope production would lead to a better understanding of factors driving viral evolution and immune escape at the population level. In this study, we identified cytosolic aminopeptidases cleavage preferences in primary cells and its impact on HIV Ag degradation into epitopes in primary human cell extracts by mass spectrometry and on epitope presentation to CTL. We observed a hierarchy of preferred amino acid cleavage by cytosolic aminopeptidases. We demonstrated that flanking mutations producing more or less cleavable motifs can increase or decrease epitope production and presentation by up to 14-fold. We found that the efficiency of epitope production correlates with cleavability of flanking residues. These in vitro findings were supported by in vivo population-level analyses of clinically derived viral sequences from 1134 antiretroviral-naive HIV-infected individuals: HLA-associated mutations immune pressures drove the selection of residues that are less cleavable by aminopeptidases predominantly at N-flanking sites, leading to reduced epitope production and immune recognition. These results underscore an important and widespread role of Ag processing mutations in HIV immune escape and identify molecular mechanisms underlying impaired epitope presentation.

Published

2012

208. HLA class I sequence-based typing using DNA recovered from frozen plasma

Author

M-J Milloy, Theresa Mo, Zabrina L. Brumme, Anh Q. Le, Manal A. Rahman, Laura A. Cotton, and Carmond Ng

Subjects

Adult, Adolescent, Sequence analysis, Base pair, Immunology, Genes, MHC Class I, Biology, Polymerase Chain Reaction, law.invention, chemistry.chemical_compound, Young Adult, law, Immunology and Allergy, Humans, Typing, Child, Polymerase chain reaction, Alleles, Cryopreservation, Base Sequence, Histocompatibility Testing, DNA, Sequence Analysis, DNA, Molecular biology, genomic DNA, chemistry, Nucleic acid, Leukocytes, Mononuclear, Nested polymerase chain reaction

Abstract

We describe a rapid, reliable and cost-effective method for intermediate-to-high-resolution sequence-based HLA class I typing using frozen plasma as a source of genomic DNA. The plasma samples investigated had a median age of 8.5 years. Total nucleic acids were isolated from matched frozen PBMC (~2.5 million) and plasma (500 μl) samples from a panel of 25 individuals using commercial silica-based kits. Extractions yielded median [IQR] nucleic acid concentrations of 85.7 [47.0-130.0]ng/μl and 2.2 [1.7-2.6]ng/μl from PBMC and plasma, respectively. Following extraction, ~1000 base pair regions spanning exons 2 and 3 of HLA-A, -B and -C were amplified independently via nested PCR using universal, locus-specific primers and sequenced directly. Chromatogram analysis was performed using commercial DNA sequence analysis software and allele interpretation was performed using a free web-based tool. HLA-A, -B and -C amplification rates were 100% and chromatograms were of uniformly high quality with clearly distinguishable mixed bases regardless of DNA source. Concordance between PBMC and plasma-derived HLA types was 100% at the allele and protein levels. At the nucleotide level, a single partially discordant base (resulting from a failure to call both peaks in a mixed base) was observed out of >46,975 bases sequenced (>99.9% concordance). This protocol has previously been used to perform HLA class I typing from a variety of genomic DNA sources including PBMC, whole blood, granulocyte pellets and serum, from specimens up to 30 years old. This method provides comparable specificity to conventional sequence-based approaches and could be applied in situations where cell samples are unavailable or DNA quantities are limiting.

Published

2012

209. Lack of association between HLA class II alleles and in vitro replication capacities of recombinant viruses encoding HIV-1 subtype C Gag-protease from chronically infected individuals

Author

Xiaojiang Gao, Mark A. Brockman, Zabrina L. Brumme, Jaclyn K. Wright, Jonathan M. Carlson, Philip J. R. Goulder, Thumbi Ndung'u, Boris Julg, Zenele Mncube, Bruce D. Walker, and Mary van der Stok

Subjects

CD4-Positive T-Lymphocytes, medicine.medical_treatment, T cell, Immunology, HIV Infections, Human leukocyte antigen, Biology, Virus Replication, Microbiology, gag Gene Products, Human Immunodeficiency Virus, law.invention, Immune system, law, Virology, medicine, Humans, Allele, Alleles, Genetics, Protease, Histocompatibility Antigens Class I, Histocompatibility Antigens Class II, Histocompatibility, medicine.anatomical_structure, Viral replication, Insect Science, Recombinant DNA, HIV-1, Pathogenesis and Immunity, Peptide Hydrolases

Abstract

It is unknown whether favorable HLA class II alleles may attenuate HIV-1 through selection pressure in a manner similar to that of protective HLA class I alleles. We investigated the relationship between HLA class II alleles and in vitro replication capacities of recombinant viruses encoding HIV-1 subtype C Gag-protease from chronically infected individuals. No associations were found between individual alleles and lower replication capacity, suggesting no significant HIV-1 attenuation by HLA class II-restricted Gag-specific CD4 + T cell immune pressure.

Published

2012

210. Characteristics and Outcomes of Initial Virologic Suppressors during Analytic Treatment Interruption in a Therapeutic HIV-1 gag Vaccine Trial

Author

Chanson J. Brumme, Mary Carrington, Hongying Wang, Bruce D. Walker, Robert T. Schooley, Michael M. Lederman, John Spritzler, Zabrina L. Brumme, Daniel R. Kuritzkes, Kathleen A. Medvik, Jonathan Z. Li, and Ensoli, Barbara

Subjects

CD4-Positive T-Lymphocytes, Male, Viral Diseases, Cell, Programmed Cell Death 1 Receptor, lcsh:Medicine, gag Gene Products, Human Immunodeficiency Virus, Placebos, 0302 clinical medicine, CTLA-4 Antigen, 030212 general & internal medicine, lcsh:Science, AIDS Vaccines, Vaccines, Synthetic, 0303 health sciences, Vaccines, Multidisciplinary, medicine.diagnostic_test, Viral Vaccine, Vaccination, Middle Aged, Flow Cytometry, 3. Good health, medicine.anatomical_structure, Infectious Diseases, Treatment Outcome, Medicine, HIV/AIDS, Cytokines, Female, Infection, Viral load, Sequence Analysis, Human Immunodeficiency Virus, Research Article, Biotechnology, Adult, General Science & Technology, Clinical Trials and Supportive Activities, Molecular Sequence Data, Biology, Microbiology, Flow cytometry, Vaccine Related, 03 medical and health sciences, Immune system, AIDS Clinical Trials Group A5197 Study Team, Immunity, Clinical Research, Virology, medicine, Humans, gag Gene Products, 030304 developmental biology, lcsh:R, Synthetic, Vaccine trial, HIV, Reproducibility of Results, Sequence Analysis, DNA, DNA, CD4 Lymphocyte Count, Good Health and Well Being, Immune System, Immunology, HIV-1, lcsh:Q, Clinical Immunology, Immunization

Abstract

Background: In the placebo-controlled trial ACTG A5197, a trend favoring viral suppression was seen in the HIV-1-infected subjects who received a recombinant Ad5 HIV-1 gag vaccine. Objective: To identify individuals with initial viral suppression (plasma HIV-1 RNA set point ,3.0 log10 copies/ml) during the analytic treatment interruption (ATI) and evaluate the durability and correlates of virologic control and characteristics of HIV sequence evolution. Methods: HIV-1 gag and pol RNA were amplified and sequenced from plasma obtained during the ATI. Immune responses were measured by flow cytometric analysis and intracellular cytokine expression assays. Characteristics of those with and without initial viral suppression were compared using the Wilcoxon rank sum and Fisher’s exact tests. Results: Eleven out of 104 participants (10.6%) were classified as initial virologic suppressors, nine of whom had received the vaccine. Initial virologic suppressors had significantly less CD4+ cell decline by ATI week 16 as compared to non-suppressors (median 7 CD4+ cell gain vs. 247 CD4+ cell loss, P=0.04). However, of the ten initial virologic suppressors with a pVL at ATI week 49, only three maintained pVL ,3.0 log10 copies/ml. HIV-1 Gag-specific CD4+ interferon-c responses were not associated with initial virologic suppression and no evidence of vaccine-driven HIV sequence evolution was detected. Participants with initial virologic suppression were found to have a lower percentage of CD4+ CTLA-4+ cells prior to treatment interruption, but a greater proportion of HIV-1 Gag-reactive CD4+ TNF-a+ cells expressing either CTLA-4 or PD-1. Conclusions: Among individuals participating in a rAd5 therapeutic HIV-1 gag vaccine trial, initial viral suppression was found in a subset of patients, but this response was not sustained. The association between CTLA-4 and PD-1 expression on CD4+ T cells and virologic outcome warrants further study in trials of other therapeutic vaccines in development. Trial Registration: ClinicalTrials.gov NCT00080106

Published

2012

211. Definition of the viral targets of protective HIV-1-specific T cell responses

Author

Bruce D. Walker, Beatriz Mothe, Jorge Sanchez, Vanessa Bach, Philip J. R. Goulder, James J. Szinger, Otto O. Yang, Chanson J. Brumme, William H. Hildebrand, Christoph Berger, Victor Sanchez-Merino, Todd M. Allen, Zabrina L. Brumme, Cristina Miranda, Bonaventura Clotet, Rosario Zuñiga, Morgane Rolland, David Heckerman, F. Javier Ibarrondo, Anuska Llano, Susana Pérez-Álvarez, Guadalupe Gómez, Bette T. Korber, José M. Gatell, Marilu Farfan, Marcus Daniels, Javier Martinez-Picado, James I. Mullins, Maria C. Puertas, Christian Brander, Jennifer Zamarreño, Universitat Politècnica de Catalunya. Departament d'Estadística i Investigació Operativa, and Universitat Politècnica de Catalunya. GREMA - Grup de Recerca en Estadística Matemàtica i les seves Aplicacions

Subjects

Male, Biologia, HIV specific CTL, immune correlate, T-Lymphocytes, lcsh:Medicine, HIV Infections, Virus Replication, gag Gene Products, Human Immunodeficiency Virus, Epitope, Conserved sequence, Cohort Studies, 0302 clinical medicine, Peru, HIV vaccine, Conserved Sequence, Medicine(all), epitope, 0303 health sciences, General Medicine, Viral Load, 3. Good health, HLA, medicine.anatomical_structure, 030220 oncology & carcinogenesis, vaccine immunogen design, Viral load, clade B, functional avidity, clade C, T cell, Human leukocyte antigen, Biology, General Biochemistry, Genetics and Molecular Biology, Genetic Heterogeneity, 03 medical and health sciences, Species Specificity, stomatognathic system, medicine, Humans, Amino Acid Sequence, Alleles, 92 Biology and other natural sciences::92C Physiological, cellular and medical topics [Classificació AMS], 030304 developmental biology, Matemàtiques i estadística::Estadística aplicada::Estadística biosanitària [Àrees temàtiques de la UPC], Biochemistry, Genetics and Molecular Biology(all), Research, lcsh:R, Histocompatibility Antigens Class I, Virology, stomatognathic diseases, CTL, Viral replication, Multivariate Analysis, Immunology, HIV-1, Peptides, entropy

Abstract

Background The efficacy of the CTL component of a future HIV-1 vaccine will depend on the induction of responses with the most potent antiviral activity and broad HLA class I restriction. However, current HIV vaccine designs are largely based on viral sequence alignments only, not incorporating experimental data on T cell function and specificity. Methods Here, 950 untreated HIV-1 clade B or -C infected individuals were tested for responses to sets of 410 overlapping peptides (OLP) spanning the entire HIV-1 proteome. For each OLP, a "protective ratio" (PR) was calculated as the ratio of median viral loads (VL) between OLP non-responders and responders. Results For both clades, there was a negative relationship between the PR and the entropy of the OLP sequence. There was also a significant additive effect of multiple responses to beneficial OLP. Responses to beneficial OLP were of significantly higher functional avidity than responses to non-beneficial OLP. They also had superior in-vitro antiviral activities and, importantly, were at least as predictive of individuals' viral loads than their HLA class I genotypes. Conclusions The data thus identify immunogen sequence candidates for HIV and provide an approach for T cell immunogen design applicable to other viral infections.

Published

2011

212. Whole genome deep sequencing of HIV-1 reveals the impact of early minor variants upon immune recognition during acute infection

Author

Alexander R. Macalalad, Jenna Rychert, Chanson J. Brumme, Adrianne D. Gladden, Bruce W. Birren, Sarah Young, Bruce D. Walker, Suzane Bazner, Heiko Jessen, Damien C. Tully, Karen L. Axten, Monica Casali, Andrew Berical, Allyson K. Bloom, Jake P. Tinsley, Christian Brander, Niall J. Lennon, Joshua Z. Levin, Yaoyu E. Wang, Zabrina L. Brumme, Christoph Hess, Laura Battis, Christine M. Malboeuf, Florencia Pereyra, Michael Kemper, Michael C Zody, Hendrik Streeck, Carmen Zedlack, Sharvari Gujja, Huldrych F. Günthard, Olivier Gasser, Eric S. Rosenberg, Todd M. Allen, Kenneth H. Mayer, Terrance Shea, Sante Gnerre, Rachel L. Erlich, Ruchi M. Newman, Lisa Green, Marcus Altfeld, Tim Dudek, Matthew R. Henn, Patrick Charlebois, Qiandong Zeng, Elizabeth M. Ryan, Christian L. Boutwell, Karen A. Power, Aaron M. Berlin, and University of Zurich

Subjects

Viral Diseases, 2405 Parasitology, HIV Infections, CD8-Positive T-Lymphocytes, 10234 Clinic for Infectious Diseases, Biology (General), Oligonucleotide Array Sequence Analysis, Genetics, 0303 health sciences, Viral Vaccine, 2404 Microbiology, 3. Good health, medicine.anatomical_structure, Infectious Diseases, Viral evolution, RNA, Viral, Medicine, Viral load, Research Article, QH301-705.5, T cell, Immune Cells, Immunology, 610 Medicine & health, Viremia, Viral quasispecies, Genome, Viral, Biology, Microbiology, Deep sequencing, 03 medical and health sciences, Immune system, 1311 Genetics, Virology, 1312 Molecular Biology, medicine, Humans, Molecular Biology, 030304 developmental biology, Immune Evasion, 2403 Immunology, 030306 microbiology, Sequence Analysis, RNA, Immunity, Genetic Variation, HIV, Viral Vaccines, RC581-607, medicine.disease, Genomic Structural Variation, 2406 Virology, HIV-1, Parasitology, Clinical Immunology, Immunologic diseases. Allergy, Genome-Wide Association Study

Abstract

Deep sequencing technologies have the potential to transform the study of highly variable viral pathogens by providing a rapid and cost-effective approach to sensitively characterize rapidly evolving viral quasispecies. Here, we report on a high-throughput whole HIV-1 genome deep sequencing platform that combines 454 pyrosequencing with novel assembly and variant detection algorithms. In one subject we combined these genetic data with detailed immunological analyses to comprehensively evaluate viral evolution and immune escape during the acute phase of HIV-1 infection. The majority of early, low frequency mutations represented viral adaptation to host CD8+ T cell responses, evidence of strong immune selection pressure occurring during the early decline from peak viremia. CD8+ T cell responses capable of recognizing these low frequency escape variants coincided with the selection and evolution of more effective secondary HLA-anchor escape mutations. Frequent, and in some cases rapid, reversion of transmitted mutations was also observed across the viral genome. When located within restricted CD8 epitopes these low frequency reverting mutations were sufficient to prime de novo responses to these epitopes, again illustrating the capacity of the immune response to recognize and respond to low frequency variants. More importantly, rapid viral escape from the most immunodominant CD8+ T cell responses coincided with plateauing of the initial viral load decline in this subject, suggestive of a potential link between maintenance of effective, dominant CD8 responses and the degree of early viremia reduction. We conclude that the early control of HIV-1 replication by immunodominant CD8+ T cell responses may be substantially influenced by rapid, low frequency viral adaptations not detected by conventional sequencing approaches, which warrants further investigation. These data support the critical need for vaccine-induced CD8+ T cell responses to target more highly constrained regions of the virus in order to ensure the maintenance of immunodominant CD8 responses and the sustained decline of early viremia., Author Summary The ability of HIV-1 and other highly variable pathogens to rapidly mutate to escape vaccine-induced immune responses represents a major hurdle to the development of effective vaccines to these highly persistent pathogens. Application of next-generation or deep sequencing technologies to the study of host pathogens could significantly improve our understanding of the mechanisms by which these pathogens subvert host immunity, and aid in the development of novel vaccines and therapeutics. Here, we developed a 454 deep sequencing approach to enable the sensitive detection of low-frequency viral variants across the entire HIV-1 genome. When applied to the acute phase of HIV-1 infection we observed that the majority of early, low frequency mutations represented viral adaptations to host cellular immune responses, evidence of strong host immunity developing during the early decline of peak viral load. Rapid viral escape from the most dominant immune responses however correlated with loss of this initial viral control, suggestive of the importance of mounting immune responses against more conserved regions of the virus. These data provide a greater understanding of the early evolutionary events subverting the ability of host immune responses to control early HIV-1 replication, yielding important insight into the design of more effective vaccine strategies.

Published

2011

213. Impairment of viral replication capacity by nef alleles from HIV elite controllers

Author

Tristan J. Markle, Yoko Ogata, Bruce D. Walker, Toshiyuki Miura, Hirohito Otsuka, Philip Mwimanzi, Michiyo Tokunaga, Zabrina L. Brumme, Takamasa Ueno, Florencia Pereyra, Mark A. Brockman, and Eric Martin

Subjects

Infectivity, lcsh:Immunologic diseases. Allergy, viruses, Clone (cell biology), virus diseases, Viremia, Biology, medicine.disease, Virology, Virus, law.invention, Infectious Diseases, Plasmid, Viral replication, law, Poster Presentation, Recombinant DNA, biology.protein, medicine, Antibody, lcsh:RC581-607

Abstract

Background Elite controllers (EC) are HIV-1 infected persons who can spontaneously control viremia to extremely low levels. Because it is known that nef is required for HIV1 replication and pathogenesis in vivo, we wish to clarify how HIV-1 nef plays a role in acquiring EC phenotype. Materials and methods Viral RNAs were extracted from plasma samples of 45 ECs and 48 chronic progressors (CP) and used for amplification of nef by RT-PCR. The amplified products were cloned into a plasmid and subsequently sequenced. A representative nef clone was selected for each patient and cloned into an NL43 proviral plasmid backbone. Infectious recombinant viruses were prepared by transfecting 293T cells with these resultant proviral clones and tested for their viral replication capacity in PBMCs obtained from multiple healthy donors. Viral replication was monitored by measuring the concentration of p24 Gag in the culture supernatant by p24 ELISA every 3 days. The same virus stocks were further tested for their infectivity using TZM-bl cells. Results All nef alleles isolated from EC and CP had intact ORFs. Phylogenetic analysis revealed no specific lineage or clustering, suggesting the absence of common genetic defects in EC-derived nef alleles. All viruses expressing patient-derived nef showed a wide range of viral replication in PBMC, confirming the importance of nef alleles in the enhancement of viral replication capacity. The viruses harboring EC-derived nef replicated and peaked on Day 12 after infection or even later; whereas the viruses harboring CP-derived nef peaked on Day 9. Also, the peak level of p24 values was significantly lower in the EC-nef viruses than in the CP-nef viruses. Because Nef activity is highly dependent on PBMC donors, we tested 4 different donors’ PBMC and compared the initial burst of their viral replication at Day 9. In all donors’PBMC, viruses carrying EC-nef displayed lower p24 values than those carrying CP-nef, suggesting that the viral replication capacity was much impaired by nef alleles in EC. Corroboratively, in viral infectivity assay in TZM-bl cells, the EC-nef viruses showed significantly lower infectivity than the CP-nef viruses. Conclusion

Published

2011

214. Progression to AIDS in South Africa Is Associated with both Reverting and Compensatory Viral Mutations

Author

Dewald Steyn, Zabrina L. Brumme, Christopher S. W. Tang, Stephen Hickling, Cloete van Vuuren, David Heckerman, Jonathan M. Carlson, Philip J. R. Goulder, Thumbi Ndung'u, Swati Mishra, Toshiyuki Miura, Bruce D. Walker, Mark A. Brockman, Rodney E. Phillips, Dominique Goedhals, Christopher J. Seebregts, Kuan-Hsiang Gary Huang, John Frater, and Paul Klenerman

Subjects

Enzyme-Linked Immunospot Assay, T cell, viruses, Sexually Transmitted Diseases, lcsh:Medicine, Disease, Biology, gag Gene Products, Human Immunodeficiency Virus, Epitope, 03 medical and health sciences, South Africa, Immune system, medicine, Humans, nef Gene Products, Human Immunodeficiency Virus, lcsh:Science, 030304 developmental biology, 0303 health sciences, Acquired Immunodeficiency Syndrome, Multidisciplinary, Polymorphism, Genetic, 030306 microbiology, ELISPOT, lcsh:R, Histocompatibility Antigens Class I, Virology, 3. Good health, CD4 Lymphocyte Count, AIDS, medicine.anatomical_structure, Infectious Diseases, Viral replication, pol Gene Products, Human Immunodeficiency Virus, Immunology, Mutation, biology.protein, Disease Progression, Medicine, lcsh:Q, Antibody, Viral load, Research Article

Abstract

We lack the understanding of why HIV-infected individuals in South Africa progress to AIDS. We hypothesised that in end-stage disease there is a shifting dynamic between T cell imposed immunity and viral immune escape, which, through both compensatory and reverting viral mutations, results in increased viral fitness, elevated plasma viral loads and disease progression. We explored how T cell responses, viral adaptation and viral fitness inter-relate in South African cohorts recruited from Bloemfontein, the Free State (n=278) and Durban, KwaZulu-Natal (n=775). Immune responses were measured by (Gamma)-interferon ELISPOT assays. HLA-associated viral polymorphisms were determined using phylogenetically corrected techniques, and viral replication capacity (VRC) was measured by comparing the growth rate of gag-protease recombinant viruses against recombinant NL4-3 viruses. We report that in advanced disease (CD4 counts

Published

2011

215. P762 TEMPORAL CHANGES IN HEPATITIS C VIRUS GENOTYPE 3A DISTRIBUTION AMONG PEOPLE WHO INJECT DRUGS IN VANCOUVER, CANADA

Author

Richard Harrigan, G.J. Dore, Zabrina L. Brumme, M. Krajden, Jason Grebely, Art F. Y. Poon, Tanya L. Applegate, V. Dias Lima, Sabina Dobrer, Thomas Kerr, Jeffrey B. Joy, Brendan Jacka, M.-J. Milloy, Andrea D. Olmstead, F. Lamoury, J. S. G. Montaner, Brandon D.L. Marshall, Conan K. Woods, Kora DeBeck, and Evan Wood

Subjects

Hepatology, Hepatitis C virus genotype, Distribution (pharmacology), Biology, Virology

Published

2014

216. Reduced replication capacity of NL4-3 recombinant viruses encoding reverse transcriptase-integrase sequences from HIV-1 elite controllers

Author

Zabrina L. Brumme, Mark A. Brockman, Florencia Pereyra, Chanson J. Brumme, David Heckerman, Alicja Trocha, Carl M. Kadie, Bruce D. Walker, Chun Li, Pamela C. Rosato, Brian L. Block, Todd M. Allen, Jennifer Sela, Eric Martin, Tristan J. Markle, and Toshiyuki Miura

Subjects

viruses, Viremia, HIV Infections, HIV Integrase, medicine.disease_cause, Virus Replication, Virus, Article, law.invention, HIV Long-Term Survivors, law, medicine, Humans, Pharmacology (medical), Genetics, Recombination, Genetic, Mutation, biology, Virulence, biology.organism_classification, medicine.disease, Virology, Reverse transcriptase, HIV Reverse Transcriptase, Integrase, Infectious Diseases, Viral replication, Lentivirus, Recombinant DNA, biology.protein, HIV-1

Abstract

Background: Identifying viral and host determinants of HIV-1 elite control may help inform novel therapeutic and/or vaccination strategies. Previously, we observed decreased replication capacity in controller-derived viruses suggesting that fitness consequences of human leukocyte antigen (HLA) class I-associated escape mutations in Gag may contribute to this phenotype. This study examines whether similar functional defects occur in Pol proteins of elite controllers. Methods: Recombinant NL4-3 viruses encoding plasma RNA-derived reverse transcriptase-integrase sequences from 58 elite controllers and 50 untreated chronic progressors were constructed, and replication capacity measured in vitro using a green fluorescent protein (GFP) reporter T-cell assay. Sequences were analyzed for drug resistance and HLA-associated viral polymorphisms. Results: Controller-derived viruses displayed significantly lower replication capacity compared with those from progressors (P < 0.0001). Among controllers, the most attenuated viruses were generated from individuals expressing HLA-B * 57 or B * 51. In viruses from B * 57+ progressors (n = 8), a significant inverse correlation was observed between B * 57-associated reverse transcriptase-integrase escape mutations and replication capacity (R = —0.89; P = 0.003); a similar trend was observed in B * 57+ controller-derived viruses (n = 20, R = -0.36; P = 0.08). Conclusions: HIV-1 Pol function seemed to be compromised in elite controllers. As observed previously for Gag, HLA-associated immune pressure in Pol may contribute to viral attenuation and subsequent control of viremia.

Published

2010

217. In vitro selection of clinically relevant bevirimat resistance mutations revealed by 'deep' sequencing of serially passaged, quasispecies-containing recombinant HIV-1

Author

P. Richard Harrigan, Art F. Y. Poon, Peter K. Cheung, Zabrina L. Brumme, David J.H.F. Knapp, and Mark A. Brockman

Subjects

Microbiology (medical), Anti-HIV Agents, Population, Mutation, Missense, Drug resistance, Viral quasispecies, Biology, gag Gene Products, Human Immunodeficiency Virus, Deep sequencing, chemistry.chemical_compound, Virology, Drug Resistance, Viral, Humans, Selection, Genetic, Serial Passage, education, education.field_of_study, Wild type, High-Throughput Nucleotide Sequencing, Succinates, Amplicon, Resistance mutation, Molecular biology, Triterpenes, chemistry, HIV-1, RNA, Viral, Bevirimat

Abstract

Initial in vitro studies of bevirimat resistance failed to observe mutations in the clinically significant QVT motif in SP1 of HIV-1 gag . This study presents a novel screening method involving mixed, clinically derived gag-protease recombinant HIV-1 samples to more accurately mimic the selection of resistance seen in vivo . Bevirimat resistance was investigated via population-based sequencing performed with a large, initially antiretroviral-naïve cohort before ( n = 805) and after ( n = 355) standard HIV therapy (without bevirimat). The prevalence of any polymorphism in the motif comprising Q, V, and T was ∼6%, 29%, and 12%, respectively, and did not change appreciably over the course of therapy. From these samples, three groups of 10 samples whose bulk sequences were wild type at the QVT motif were used to generate gag-protease recombinant viruses that captured the existing diversity. Groups were mixed and passaged with various bevirimat concentrations for 9 weeks. gag variations were assessed by amplicon-based “deep” sequencing using a GS FLX sequencer (Roche). Unscreened mutations were present in all groups, and a V370A minority not originally detected by bulk sequencing was present in one group. V370A, occurring together with another preexisting, unscreened resistance mutation, was selected in all groups in the presence of a bevirimat concentration above 0.1 μM. For the two groups with V370A levels below consistent detectability by deep sequencing, the initial selection of V370A required 3 to 4 weeks of exposure to a narrow range of bevirimat concentrations, whereas for the group with the V370A minority, selection occurred immediately. This approach provides quasispecies diversity that facilitates the selection of mutations observed in clinical trials and, coupled with deep sequencing, could represent an efficient in vitro screening method for detecting resistance mutations.

Published

2010

218. Early Selection in Gag by Protective HLA Alleles Contributes to Reduced HIV-1 Replication Capacity That May Be Largely Compensated for in Chronic Infection▿ †

Author

Mark A. Brockman, Eric S. Rosenberg, Zabrina L. Brumme, Carl M. Kadie, Tristan J. Markle, Jennifer Sela, Hendrik Streeck, Toshiyuki Miura, Anthony D. Kelleher, Marcus Altfeld, Jonathan M. Carlson, Todd M. Allen, Bruce D. Walker, Pamela C. Rosato, Martin Markowitz, P. Richard Harrigan, Chanson J. Brumme, David Heckerman, and Heiko Jessen

Subjects

Male, Immunology, Molecular Sequence Data, HIV Infections, Human leukocyte antigen, Biology, medicine.disease_cause, Virus Replication, Microbiology, gag Gene Products, Human Immunodeficiency Virus, Virus, Pathogenesis, Cohort Studies, Virology, medicine, Humans, Allele, Alleles, Mutation, Group-specific antigen, CD4 Lymphocyte Count, Chronic infection, Viral replication, HLA-B Antigens, Insect Science, Chronic Disease, HIV-1, Pathogenesis and Immunity

Abstract

Mutations that allow escape from CD8 T-cell responses are common in HIV-1 and may attenuate pathogenesis by reducing viral fitness. While this has been demonstrated for individual cases, a systematic investigation of the consequence of HLA class I-mediated selection on HIV-1 in vitro replication capacity (RC) has not been undertaken. We examined this question by generating recombinant viruses expressing plasma HIV-1 RNA-derived Gag-Protease sequences from 66 acute/early and 803 chronic untreated subtype B-infected individuals in an NL4-3 background and measuring their RCs using a green fluorescent protein (GFP) reporter CD4 T-cell assay. In acute/early infection, viruses derived from individuals expressing the protective alleles HLA-B*57, -B*5801, and/or -B*13 displayed significantly lower RCs than did viruses from individuals lacking these alleles ( P < 0.05). Furthermore, acute/early RC inversely correlated with the presence of HLA-B-associated Gag polymorphisms ( R = −0.27; P = 0.03), suggesting a cumulative effect of primary escape mutations on fitness during the first months of infection. At the chronic stage of infection, no strong correlations were observed between RC and protective HLA-B alleles or with the presence of HLA-B-associated polymorphisms restricted by protective alleles despite increased statistical power to detect these associations. However, RC correlated positively with the presence of known compensatory mutations in chronic viruses from B*57-expressing individuals harboring the Gag T242N mutation ( n = 50; R = 0.36; P = 0.01), suggesting that the rescue of fitness defects occurred through mutations at secondary sites. Additional mutations in Gag that may modulate the impact of the T242N mutation on RC were identified. A modest inverse correlation was observed between RC and CD4 cell count in chronic infection ( R = −0.17; P < 0.0001), suggesting that Gag-Protease RC could increase over the disease course. Notably, this association was stronger for individuals who expressed B*57, B*58, or B*13 ( R = −0.27; P = 0.004). Taken together, these data indicate that certain protective HLA alleles contribute to early defects in HIV-1 fitness through the selection of detrimental mutations in Gag; however, these effects wane as compensatory mutations accumulate in chronic infection. The long-term control of HIV-1 in some persons who express protective alleles suggests that early fitness hits may provide lasting benefits.

Published

2010

219. Efficacious Early Antiviral Activity of HIV Gag- and Pol-Specific HLA-B*2705-Restricted CD8+ T Cells ▿

Author

Rebecca Payne, Zabrina L. Brumme, Anne Edwards, Chanson J. Brumme, Henrik N. Kløverpris, Fabian Chen, Jonah B. Sacha, Stephen Hickling, Stuart Sims, Rodney E. Phillips, Lynn Riddell, Philip J. R. Goulder, Søren Buus, Graz Luzzi, and Julia G. Prado

Subjects

Cytotoxicity, Immunologic, HIV Antigens, viruses, Immunology, Molecular Sequence Data, Epitopes, T-Lymphocyte, HIV Infections, CD8-Positive T-Lymphocytes, In Vitro Techniques, Microbiology, gag Gene Products, Human Immunodeficiency Virus, Epitope, Virus, HIV Long-Term Survivors, Interleukin 21, Virology, Cytotoxic T cell, Humans, Amino Acid Sequence, HLA-B27 Antigen, AIDS Vaccines, biology, Immunodominant Epitopes, vpr Gene Products, Human Immunodeficiency Virus, Peptide Fragments, Viral replication, pol Gene Products, Human Immunodeficiency Virus, Insect Science, Mutation, biology.protein, HIV-1, Pathogenesis and Immunity, Antibody, CD8

Abstract

The association between HLA-B*2705 and the immune control of human immunodeficiency virus type 1 (HIV-1) has previously been linked to the targeting of the HLA-B*2705-restricted Gag epitope KRWIILGLNK (KK10) by CD8 + T cells. In order to better define the mechanisms of the HLA-B*2705 immune control of HIV, we first characterized the CD8 + T-cell responses of nine highly active antiretroviral therapy (HAART)-naïve B*2705-positive subjects. Unexpectedly, we observed a strong response to an HLA-B*2705-restricted Pol epitope, KRKGGIGGY (KY9), in 8/9 subjects. The magnitude of the KY9 response was only marginally lower than that of the KK10-specific response (median, 695 versus 867 spot-forming cells [SFC]/million peripheral blood mononuclear cells [PBMCs]; not significant [NS]), and viral escape mutants were observed in both KY9 and KK10, resulting from selection pressure driven by the respective CD8 + T-cell response. By comparing inhibitions of viral replication by CD8 + T cells specific for the Gag KK10, Pol KY9, and Vpr VL9 HLA-B*2705-restricted epitopes, we observed a consistent hierarchy of antiviral efficacy (Gag KK10 > Pol KY9 > Vpr VL9). This hierarchy was associated with early recognition of HIV-1-infected cells, within 6 h of infection, by KK10- and KY9-specific CD8 + T cells but not until 18 h postinfection by VL9-specific CD8 + T cells. There was no association between antiviral efficacy and proliferative capacity, cytotoxicity, polyfunctionality, or T-cell receptor (TCR) avidity. These data are consistent with previous studies indicating an important role for the B*2705-Gag KK10 response in the control of HIV but also suggest a previously unrecognized role played by the subdominant Pol-specific KY9 response in HLA-B*2705-mediated control of HIV and that the recognition of HIV-infected cells by CD8 + T cells early in the viral life cycle may be important for viral containment in HIV-infected individuals.

Published

2010

220. Impaired replication capacity of acute/early viruses in persons who become HIV controllers

Author

Zabrina L. Brumme, Chanson J. Brumme, Anthony D. Kelleher, Kim Schafer, Heiko Jessen, Eric S. Daar, Bruce D. Walker, Alicja Trocha, Pamela C. Rosato, Eric S. Rosenberg, Elizabeth Connick, Brian L. Block, Mark A. Brockman, Jennifer Sela, Aikichi Iwamoto, Florin Vaida, Susan J. Little, Martin Markowitz, Toshiyuki Miura, Daniel Kaufmann, and Florencia Pereyra

Subjects

Immunology, Molecular Sequence Data, Mutation, Missense, Viremia, HIV Infections, medicine.disease_cause, Virus Replication, Microbiology, Virus, HIV Long-Term Survivors, Virology, Drug Resistance, Viral, medicine, Humans, Mutation, biology, Histocompatibility Antigens Class I, Sequence Analysis, DNA, Viral Load, biology.organism_classification, medicine.disease, Chronic infection, Viral replication, Insect Science, Lentivirus, HIV-1, RNA, Viral, Pathogenesis and Immunity, Viral load, T-Lymphocytes, Cytotoxic

Abstract

Human immunodeficiency virus type 1 (HIV-1) controllers maintain viremia at g ag-protease chimeric viruses constructed using the earliest postinfection samples displayed significantly lower replication capacities than isolates from persons who failed to control viremia ( P = 0.0003). Protective HLA class I alleles were not enriched in these early HIV controllers, but viral sequencing revealed a significantly higher prevalence of drug resistance mutations associated with impaired viral fitness in controllers than in noncontrollers (6/15 [40.0%] versus 10/80 [12.5%], P = 0.018). Moreover, of two HLA-B57-positive (B57 + ) controllers identified, both harbored, at the earliest time point tested, signature escape mutations within Gag that likewise impair viral replication capacity. Only five controllers did not express “protective” alleles or harbor viruses with drug resistance mutations; intriguingly, two of them displayed typical B57 signature mutations (T242N), suggesting the acquisition of attenuated viruses from B57 + donors. These data indicate that acute/early stage viruses from persons who become controllers have evidence of reduced replication capacity during the initial stages of infection which is likely associated with transmitted or acquired CTL escape mutations or transmitted drug resistance mutations. These data suggest that viral dynamics during acute infection have a major impact on HIV disease outcome.

Published

2010

221. Viral adaptation to immune selection pressure by HLA class I-restricted CTL responses targeting epitopes in HIV frameshift sequences

Author

Zabrina L. Brumme, Pamela C. Rosato, P. Richard Harrigan, Chanson J. Brumme, Daniel Kaufmann, Kari L. Hartman, Christopher T. Berger, David Heckerman, Alicja Piechocka-Trocha, Jonathan M. Carlson, Christian Brander, Mark A. Brockman, and Leah M. Henry

Subjects

Male, Immunology, Reading frame, Codon, Initiator, Epitopes, T-Lymphocyte, HIV Infections, Human leukocyte antigen, Biology, CD8-Positive T-Lymphocytes, HLA-A3 Antigen, Virus Replication, Epitope, Article, Frameshift mutation, Evolution, Molecular, 03 medical and health sciences, Viral Proteins, 0302 clinical medicine, Immunology and Allergy, Humans, Frameshift Mutation, 030304 developmental biology, 0303 health sciences, Immunity, Cellular, Polymorphism, Genetic, HLA-A Antigens, HIV, Group-specific antigen, Virology, 3. Good health, CTL, Viral replication, Viral evolution, Female, Peptides, 030215 immunology

Abstract

CD8+ cytotoxic T lymphocyte (CTL)–mediated immune responses to HIV contribute to viral control in vivo. Epitopes encoded by alternative reading frame (ARF) peptides may be targeted by CTLs as well, but their frequency and in vivo relevance are unknown. Using host genetic (human leukocyte antigen [HLA]) and plasma viral sequence information from 765 HIV-infected subjects, we identified 64 statistically significant (q < 0.2) associations between specific HLA alleles and sequence polymorphisms in alternate reading frames of gag, pol, and nef that did not affect the regular frame protein sequence. Peptides spanning the top 20 HLA-associated imprints were used to test for ex vivo immune responses in 85 HIV-infected subjects and showed responses to 10 of these ARF peptides. The most frequent response recognized an HLA-A*03–restricted +2 frame–encoded epitope containing a unique A*03-associated polymorphism at position 6. Epitope-specific CTLs efficiently inhibited viral replication in vitro when viruses containing the wild-type sequence but not the observed polymorphism were tested. Mutating alternative internal start codons abrogated the CTL-mediated inhibition of viral replication. These data indicate that responses to ARF-encoded HIV epitopes are induced during natural infection, can contribute to viral control in vivo, and drive viral evolution on a population level.

Published

2010

222. HLA-Associated Viral Mutations Are Common in Human Immunodeficiency Virus Type 1 Elite Controllers

Author

P. Richard Harrigan, Chanson J. Brumme, Florencia Pereyra, Brian L. Block, Bruce D. Walker, Simon Mallal, Zabrina L. Brumme, Mina John, Alicja Trocha, Mark A. Brockman, and Toshiyuki Miura

Subjects

Author's Correction, viruses, Immunology, Mutation, Missense, Human immunodeficiency virus (HIV), Epitopes, T-Lymphocyte, HIV Infections, Type (model theory), Biology, medicine.disease_cause, gag Gene Products, Human Immunodeficiency Virus, Microbiology, HIV Long-Term Survivors, Plasma, Virology, medicine, Humans, Viremia, nef Gene Products, Human Immunodeficiency Virus, Selection, Genetic, Polymorphism, Genetic, Viral Load, Term (logic), pol Gene Products, Human Immunodeficiency Virus, Insect Science, HIV-1, Pathogenesis and Immunity, Humanities, Elite controllers

Abstract

Volume 83, no. 7, p. 3407-3412, 2009. GenBank accession numbers were erroneously omitted from the original publication. The GenBank accession numbers for the sequences derived from HIV elite controllers are {"type":"entrez-nucleotide","attrs":{"text":"EU517762","term_id":"170778583","term_text":"EU517762"}}EU517762 through {"type":"entrez-nucleotide","attrs":{"text":"EU517815","term_id":"170778689","term_text":"EU517815"}}EU517815 and {"type":"entrez-nucleotide","attrs":{"text":"EU517972","term_id":"170778854","term_text":"EU517972"}}EU517972 through {"type":"entrez-nucleotide","attrs":{"text":"EU518012","term_id":"170778934","term_text":"EU518012"}}EU518012 (as described in reference 25 of the original manuscript), {"type":"entrez-nucleotide","attrs":{"text":"EU873003","term_id":"194716779","term_text":"EU873003"}}EU873003 and {"type":"entrez-nucleotide","attrs":{"text":"EU873005","term_id":"194716783","term_text":"EU873005"}}EU873005 (as described in reference 26 of the original manuscript), and {"type":"entrez-nucleotide","attrs":{"text":"GU046566","term_id":"282935010","term_text":"GU046566"}}GU046566 through {"type":"entrez-nucleotide","attrs":{"text":"GU046604","term_id":"282935086","term_text":"GU046604"}}GU046604. The majority of the GenBank accession numbers for the sequences used to create the map of HLA-associated mutations appeared in references 7 and 9 of the original manuscript, and additional GenBank accession numbers are {"type":"entrez-nucleotide","attrs":{"text":"GQ303719","term_id":"255983903","term_text":"GQ303719"}}GQ303719 through {"type":"entrez-nucleotide","attrs":{"text":"GQ304249","term_id":"255984963","term_text":"GQ304249"}}GQ304249, {"type":"entrez-nucleotide","attrs":{"text":"GQ371216","term_id":"255985852","term_text":"GQ371216"}}GQ371216 through {"type":"entrez-nucleotide","attrs":{"text":"GQ372824","term_id":"256012799","term_text":"GQ372824"}}GQ372824, {"type":"entrez-nucleotide","attrs":{"text":"GQ398382","term_id":"255985027","term_text":"GQ398382"}}GQ398382 through {"type":"entrez-nucleotide","attrs":{"text":"GQ398387","term_id":"255985037","term_text":"GQ398387"}}GQ398387, and {"type":"entrez-nucleotide","attrs":{"text":"AY856956","term_id":"62532449","term_text":"AY856956"}}AY856956 through {"type":"entrez-nucleotide","attrs":{"text":"AY857186","term_id":"62532638","term_text":"AY857186"}}AY857186 (as described in a new publication [1]).

Published

2010

223. P09-19 LB. CTL escape mutations in gag epitopes restricted by protective HLA class I alleles cause substantial reductions in viral replication capacity

Author

Bruce D. Walker, Zabrina L. Brumme, Christian L. Boutwell, Todd M. Allen, Mark A. Brockman, Chanson J. Brumme, Marcus Altfeld, Michael Kemper, Hendrik Streeck, Timothy Dudek, Katherine Kane, and Arne Schneidewind

Subjects

lcsh:Immunologic diseases. Allergy, biology, business.industry, Human leukocyte antigen, Virology, Epitope, CTL, Infectious Diseases, Viral replication, Poster Presentation, Immunology, biology.protein, Medicine, Allele, Antibody, lcsh:RC581-607, business

Published

2009

224. P09-20 LB. Ultra-deep sequencing of full-length HIV-1 genomes identifies rapid viral evolution during acute infection

Author

Andrew Berical, Zabrina L. Brumme, Yaoyu E. Wang, Heiko Jessen, Joshua Z. Levin, Henn, Scott Anderson, K Axten, Bruce W. Birren, Karen A. Power, Todd M. Allen, Carsten Russ, Marcus Altfeld, Chad Nusbaum, Eric S. Rosenberg, Elizabeth P. Ryan, M Kemper, Rachel L. Erlich, Aaron M. Berlin, Lisa Green, Patrick Charlebois, Chanson J. Brumme, Christine M. Malboeuf, Monica Casali, Hendrik Streeck, Niall J. Lennon, L Philips, C Boutwell, Bruce D. Walker, and Andrew B. Gladden

Subjects

biology, business.industry, Human immunodeficiency virus (HIV), Acute infection, Ultra deep sequencing, medicine.disease_cause, Bioinformatics, Genome, Virology, Infectious Diseases, Viral evolution, Poster Presentation, biology.protein, Medicine, Antibody, business

Abstract

Open Access Poster presentation P09-20 LB. Ultra-deep sequencing of full-length HIV-1 genomes identifies rapid viral evolution during acute infection MR Henn1, C Boutwell3, N Lennon1, K Power3, C Malboeuf1, P Charlebois1, A Gladden3, J Levin1, M Casali1, L Philips3, A Berlin1, A Berical3, R Erlich1, S Anderson1, H Streeck3, M Kemper3, E Ryan1, Y Wang3, L Green1, K Axten3, Z Brumme3, C Brumme3, C Russ1, E Rosenberg3, H Jessen2, M Altfeld3, C Nusbaum1, B Walker3, B Birren1 and TM Allen*3

Published

2009

225. P16-41. Evidence for in vivo immune selection pressure exerted by HLA class I restricted CTL responses to anti-sense encoded HIV sequences

Author

Mark A. Brockman, Christoph Berger, C Kadie, Richard Harrigan, Zabrina L. Brumme, Jonathan M. Carlson, LM Henry, Chanson J. Brumme, Christian Brander, K Hartman, and David E. Heckerman

Subjects

lcsh:Immunologic diseases. Allergy, biology, Viral protein, business.industry, Human immunodeficiency virus (HIV), Human leukocyte antigen, Bioinformatics, medicine.disease_cause, Virology, CTL, Infectious Diseases, Protein structure, Immune system, In vivo, Poster Presentation, medicine, biology.protein, Antibody, lcsh:RC581-607, business

Abstract

Background Past studies have suggested that certain portions of the integrated HIV-1 proviral genome can be transcribed in the anti-sense direction, resulting in novel viral protein products that may provide alternative targets for the host anti-viral immune response. Little is known whether immune responses exist against antisense HIV peptides, whether they can recognize HIV infected cells and whether CTL-driven escape mutations within antisense peptides may be detectable on a population level.

Published

2009

226. Impact of select immunologic and virologic biomarkers on CD4 cell count decrease in patients with chronic HIV-1 subtype C infection: results from Sinikithemba Cohort, Durban, South Africa

Author

Zhigang Lu, Bruce D. Walker, Christina F. Thobakgale, Fundisiwe Chonco, Zabrina L. Brumme, Chantal de Pierres, Chanson J. Brumme, Kenneth A. Freedberg, Elena Losina, Mary van der Stok, Christian Brander, Thumbi Ndung'u, Mary Carrington, Yuko Yuki, Philip J. R. Goulder, Shabashini Reddy, Zenele Mncube, Nicole Frahm, Boris Julg, Karen S. Bishop, Eshia Moodley, Bingxia Wang, Kriebashne Nair, and Photini Kiepiela

Subjects

Microbiology (medical), education.field_of_study, biology, business.industry, Population, Human leukocyte antigen, biology.organism_classification, Virus, Infectious Diseases, Immunopathology, Immunology, Lentivirus, Medicine, Cytotoxic T cell, Viral disease, business, education, Viral load

Abstract

BACKGROUND: The extent to which immunologic and clinical biomarkers influence human immunodeficiency virus type 1 (HIV-1) infection outcomes remains incompletely characterized, particularly for non-B subtypes. On the basis of data supporting in vitro HIV-1 protein-specific CD8 T lymphocyte responses as correlates of immune control in cross-sectional studies, we assessed the relationship of these responses, along with established HIV-1 biomarkers, with rates of CD4 cell count decrease in individuals infected with HIV-1 subtype C. METHODS: Bivariate and multivariate mixed-effects models were used to assess the relationship of baseline CD4 cell count, plasma viral load, human leukocyte antigen (HLA) class I alleles, and HIV-1 protein-specific CD8 T cell responses with the rate of CD4 cell count decrease in a longitudinal population-based cohort of 300 therapy-naive, chronically infected adults with baseline CD4 cell counts >200 cells/mm(3) and plasma viral loads >500 copies/mL over a median of 25 months of follow-up. RESULTS: In bivariate analyses, baseline CD4 cell count, plasma viral load, and possession of a protective HLA allele correlated significantly with the rate of CD4 cell count decrease. No relationship was observed between HIV-1 protein-specific CD8 T cell responses and CD4 cell count decrease. Results from multivariate models incorporating baseline CD4 cell counts (201-350 vs >350 cells/mm(3)), plasma viral load (< or =100,000 vs >100,000 copies/mL), and HLA (protective vs not protective) yielded the ability to discriminate CD4 cell count decreases over a 10-fold range. The fastest decrease was observed among individuals with CD4 cell counts >350 cells/mm(3) and plasma viral loads >100,000 copies/mL with no protective HLA alleles (-59 cells/mm(3) per year), whereas the slowest decrease was observed among individuals with CD4 cell counts 201-350 cells/mm(3), plasma viral loads < or =100,000 copies/mL, and a protective HLA allele (-6 cells/mm(3) per year). CONCLUSIONS: The combination of plasma viral load and HLA class I type, but not in vitro HIV-1 protein-specific CD8 T cell responses, differentiates rates of CD4 cell count decrease in patients with chronic subtype-C infection better than either marker alone.

Published

2009

227. Adaptation of HIV-1 to human leukocyte antigen class I

Author

Simon Mallal, Roger L. Shapiro, Anna Duda, Zabrina L. Brumme, Masafumi Takiguchi, Sarah Fidler, Atsuko Hachiya, T. Roach, John Frater, Chanson J. Brumme, Susan Allen, Hayley Crawford, Jonathan Weber, Eric Hunter, Richard A. Kaslow, Shinichi Oka, Joseph Mulenga, David E. Heckerman, Philippa C Matthews, Rodney E. Phillips, Thumbi Ndung'u, Julia G. Prado, Rebecca Payne, Katja Pfafferott, Mamoru Fujiwara, Paul Klenerman, Philip J. R. Goulder, Nozomi Kuse, Alasdair Leslie, Hirokazu Koizumi, Anthony Ogwu, Yuka Kawashima, Marylyn M. Addo, Bruce D. Walker, S. Branch, Jianming Tang, P.R. Harrigan, Oliver G. Pybus, Hiroyuki Gatanaga, Andrew J. Prendergast, Todd M. Allen, Christian Brander, and Mina John

Subjects

Internationality, HIV Antigens, Epitopes, T-Lymphocyte, Human leukocyte antigen, CD8-Positive T-Lymphocytes, gag Gene Products, Human Immunodeficiency Virus, Epitope, Virus, Article, Cohort Studies, Acquired immunodeficiency syndrome (AIDS), medicine, HLA-B Antigens, Leukocytes, Humans, Alleles, Multidisciplinary, Polymorphism, Genetic, biology, medicine.disease, biology.organism_classification, Virology, Lentivirus, Immunology, HIV-1, Viral disease

Abstract

The rapid and extensive spread of the human immunodeficiency virus (HIV) epidemic provides a rare opportunity to witness host-pathogen co-evolution involving humans. A focal point is the interaction between genes encoding human leukocyte antigen (HLA) and those encoding HIV proteins. HLA molecules present fragments (epitopes) of HIV proteins on the surface of infected cells to enable immune recognition and killing by CD8(+) T cells; particular HLA molecules, such as HLA-B*57, HLA-B*27 and HLA-B*51, are more likely to mediate successful control of HIV infection. Mutation within these epitopes can allow viral escape from CD8(+) T-cell recognition. Here we analysed viral sequences and HLA alleles from >2,800 subjects, drawn from 9 distinct study cohorts spanning 5 continents. Initial analysis of the HLA-B*51-restricted epitope, TAFTIPSI (reverse transcriptase residues 128-135), showed a strong correlation between the frequency of the escape mutation I135X and HLA-B*51 prevalence in the 9 study cohorts (P = 0.0001). Extending these analyses to incorporate other well-defined CD8(+) T-cell epitopes, including those restricted by HLA-B*57 and HLA-B*27, showed that the frequency of these epitope variants (n = 14) was consistently correlated with the prevalence of the restricting HLA allele in the different cohorts (together, P < 0.0001), demonstrating strong evidence of HIV adaptation to HLA at a population level. This process of viral adaptation may dismantle the well-established HLA associations with control of HIV infection that are linked to the availability of key epitopes, and highlights the challenge for a vaccine to keep pace with the changing immunological landscape presented by HIV.

Published

2009

228. Phylogenetic dependency networks: inferring patterns of CTL escape and codon covariation in HIV-1 Gag

Author

Philippa C Matthews, Zabrina L. Brumme, P. Richard Harrigan, Chanson J. Brumme, Jonathan M. Carlson, Philip J. R. Goulder, Christine Rousseau, Carl M. Kadie, James I. Mullins, Bruce D. Walker, and David Heckerman

Subjects

Linkage disequilibrium, HIV Core Protein p24, HIV Infections, Linkage Disequilibrium, HLA Antigens, Biology (General), Clade, Phylogeny, Virology/Vaccines, Genetics, education.field_of_study, Ecology, Phylogenetic tree, env Gene Products, Human Immunodeficiency Virus, Genes, gag, Computational Biology/Evolutionary Modeling, Virology/Virus Evolution and Symbiosis, Computational Theory and Mathematics, Virology/Immunodeficiency Viruses, Modeling and Simulation, Viral evolution, Genetics and Genomics/Genetics of the Immune System, Genetics and Genomics/Comparative Genomics, Databases, Nucleic Acid, Algorithms, Research Article, QH301-705.5, Population, Human leukocyte antigen, Virology/Immune Evasion, Biology, Evolution, Molecular, Cellular and Molecular Neuroscience, Phylogenetics, Humans, Computer Simulation, Selection, Genetic, Codon, education, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, Analysis of Variance, Decision Trees, Genetic Variation, HIV, Peptide Fragments, Mutation, T-Lymphocytes, Cytotoxic

Abstract

HIV avoids elimination by cytotoxic T-lymphocytes (CTLs) through the evolution of escape mutations. Although there is mounting evidence that these escape pathways are broadly consistent among individuals with similar human leukocyte antigen (HLA) class I alleles, previous population-based studies have been limited by the inability to simultaneously account for HIV codon covariation, linkage disequilibrium among HLA alleles, and the confounding effects of HIV phylogeny when attempting to identify HLA-associated viral evolution. We have developed a statistical model of evolution, called a phylogenetic dependency network, that accounts for these three sources of confounding and identifies the primary sources of selection pressure acting on each HIV codon. Using synthetic data, we demonstrate the utility of this approach for identifying sites of HLA-mediated selection pressure and codon evolution as well as the deleterious effects of failing to account for all three sources of confounding. We then apply our approach to a large, clinically-derived dataset of Gag p17 and p24 sequences from a multicenter cohort of 1144 HIV-infected individuals from British Columbia, Canada (predominantly HIV-1 clade B) and Durban, South Africa (predominantly HIV-1 clade C). The resulting phylogenetic dependency network is dense, containing 149 associations between HLA alleles and HIV codons and 1386 associations among HIV codons. These associations include the complete reconstruction of several recently defined escape and compensatory mutation pathways and agree with emerging data on patterns of epitope targeting. The phylogenetic dependency network adds to the growing body of literature suggesting that sites of escape, order of escape, and compensatory mutations are largely consistent even across different clades, although we also identify several differences between clades. As recent case studies have demonstrated, understanding both the complexity and the consistency of immune escape has important implications for CTL-based vaccine design. Phylogenetic dependency networks represent a major step toward systematically expanding our understanding of CTL escape to diverse populations and whole viral genes., Author Summary One of the enduring challenges facing HIV vaccine design is the remarkable rate of viral mutation and adaptation that limits the ability of the immune system to mount a lasting effective response. This rapid rate of mutation leads to extensive within- and between-host viral diversity that makes creation of a broadly reactive vaccine difficult. A first step in overcoming this challenge is to identify consistent patterns in viral adaptation. Recently, several studies have analyzed large groups of HIV-infected individuals and looked for correlations between HIV polymorphisms and the HLA class I alleles that restrict the cellular immune response. Here, we point out a limitation of previous approaches: correlations among HLA alleles and HIV codons lead to statistical confounding if not taken into consideration. In response, we develop two statistical models of evolution that explicitly represent stochastic selection pressure from multiple sources. After validating these models on synthetic data, we analyze the patterns of immune escape in a multicenter cohort of over 1000 individuals. Our results identify a dense network of interactions between HLA alleles and HIV codons, as well as among HIV codons, reflecting both a complexity and a promising consistency in the way that HIV adapts to the human immune response.

Published

2008

229. Human leukocyte antigen-specific polymorphisms in HIV-1 Gag and their association with viral load in chronic untreated infection

Author

P. Richard Harrigan, Jonathan M. Carlson, Carl M. Kadie, Chanson J. Brumme, Nicole Frahm, Zabrina L. Brumme, David Heckerman, Christian Brander, Iris Tao, Bruce D. Walker, Sharon Szeto, and Dennison Chan

Subjects

Immunology, Population, Molecular Sequence Data, Genes, MHC Class I, Viremia, HIV Infections, Human leukocyte antigen, gag Gene Products, Human Immunodeficiency Virus, medicine, Immunology and Allergy, Humans, Amino Acid Sequence, education, education.field_of_study, Polymorphism, Genetic, biology, Viral Load, biology.organism_classification, medicine.disease, Virology, CD4 Lymphocyte Count, CTL, Infectious Diseases, Cross-Sectional Studies, Viral evolution, Lentivirus, Chronic Disease, HIV-1, Viral disease, Viral load, T-Lymphocytes, Cytotoxic

Abstract

OBJECTIVE Selection of specific human leukocyte antigen (HLA)-restricted cytotoxic T-lymphocyte (CTL) escape mutations in key Gag epitopes has been associated with loss of HIV immune control on an individual basis. Here we undertake a population-based identification of HLA-associated polymorphisms in Gag and investigate their relationship with plasma viral load. DESIGN Cross-sectional analysis of 567 chronically HIV subtype B-infected, treatment-naive individuals. METHODS HLA class I-associated Gag substitutions were identified using phylogenetically corrected analysis methods featuring a multivariate adjustment for HLA linkage disequilibrium and a q-value correction for multiple tests. Presence of HLA-associated substitutions and markers of HIV disease status were correlated using Spearman's rank test. RESULTS We have created a gene-wide map of HLA class I-associated substitutions in HIV-1 subtype B Gag. This features 111 HLA-associated substitutions occurring at 51 of 500 Gag codons, more than 50% of which occur within published and/or putative HLA-restricted CTL epitopes. A modest inverse correlation was observed between the total number of HLA-associated Gag polymorphic sites within each individual and plasma viral load in chronic untreated infection (R = -0.17, P < 0.0001), supporting the hypothesis that a broad ability to target Gag in vivo contributes to viral control. A modest positive correlation was observed between the proportion of these sites exhibiting HLA-associated substitutions and plasma viral load (R = 0.09, P = 0.03), consistent with a loss of viremia control with the accumulation of CTL escape mutations. CONCLUSION Results contribute to our understanding of immune-driven viral adaptation and suggest that the accumulation of CTL escape mutations in Gag results in clinically detectable consequences at the population level. These data have implications for HIV vaccines.

Published

2008

230. Genetic Characterization of Human Immunodeficiency Virus Type 1 in Elite Controllers: Lack of Gross Genetic Defects or Common Amino Acid Changes▿

Author

Yaoyu E. Wang, Brett Baker, Alicja Trocha, Jonathan M. Carlson, Todd M. Allen, Zabrina L. Brumme, Alissa C. Rothchild, David Heckerman, Marylyn M. Addo, Mark A. Brockman, Chanson J. Brumme, Theresa Flynn, Bin Li, Florencia Pereyra, Toshiyuki Miura, Bruce D. Walker, Arne Schneidewind, and Brian L. Block

Subjects

viruses, Immunology, Population, Gene Products, gag, Viremia, Genome, Viral, Virus Replication, Microbiology, Virus, Gene Products, nef, Cohort Studies, Sequence Analysis, Protein, Virology, medicine, Humans, Amino Acid Sequence, education, Codon, Gene, Phylogeny, Sequence Deletion, Genetics, education.field_of_study, biology, Base Sequence, Sequence Analysis, RNA, Sequence Analysis, DNA, Viral Load, biology.organism_classification, medicine.disease, Viral replication, Insect Science, Lentivirus, HIV-1, Pathogenesis and Immunity, RNA, Viral, Viral disease, Viral load

Abstract

Despite reports of viral genetic defects in persons who control human immunodeficiency virus type 1 (HIV-1) in the absence of antiviral therapy, the extent to which such defects contribute to the long-term containment of viremia is not known. Most previous studies examining for such defects have involved small numbers of subjects, primarily focused on subjects expressing HLA-B57, or have examined single viral genes, and they have focused on cellular proviral DNA rather than plasma viral RNA sequences. Here, we attempted viral sequencing from 95 HIV-1 elite controllers (EC) who maintained plasma viral loads of nef was sequenced, only three cases of nef deletions were identified, and gross genetic defects were rarely observed in other HIV-1 coding genes. In a codon-by-codon comparison between EC and persons with progressive infection, correcting for HLA bias and coevolving secondary mutations, a significant difference was observed at only three codons in Gag, all three of which represented the historic population consensus amino acid at the time of infection. These results indicate that the spontaneous control of HIV replication is not attributable to shared viral genetic defects or shared viral polymorphisms.

Published

2008

231. Antigen Load and Viral Sequence Diversification Determine the Functional Profile of HIV-1-Specific CD8+ T Cells

Author

Bruce D. Walker, Eric S. Rosenberg, Zabrina L. Brumme, Hendrik Streeck, Marcus Altfeld, Chanson J. Brumme, Todd M. Allen, Angela Meier, Galit Alter, Kristin W. Cohen, Jonathan S. Jolin, and Michael Anastario

Subjects

Male, T cell, Immunology, HIV Infections, Biology, CD8-Positive T-Lymphocytes, Virus Replication, Epitope, 03 medical and health sciences, Epitopes, 0302 clinical medicine, Immune system, Antigen, medicine, HIV Infection/AIDS, Cytotoxic T cell, Humans, Immunology and Allergy, Antigens, Viral, 030304 developmental biology, Research in Translation, 0303 health sciences, General Medicine, Sequence Analysis, DNA, Viral Load, Flow Cytometry, Virology, 3. Good health, medicine.anatomical_structure, Phenotype, Infectious Diseases, Viral replication, Anti-Retroviral Agents, HIV-1, Medicine, Female, Peptides, Viral load, CD8, 030215 immunology

Abstract

BackgroundVirus-specific CD8(+) T lymphocytes play a key role in the initial reduction of peak viremia during acute viral infections, but display signs of increasing dysfunction and exhaustion under conditions of chronic antigen persistence. It has been suggested that virus-specific CD8(+) T cells with a "polyfunctional" profile, defined by the capacity to secrete multiple cytokines or chemokines, are most competent in controlling viral replication in chronic HIV-1 infection. We used HIV-1 infection as a model of chronic persistent viral infection to investigate the process of exhaustion and dysfunction of virus-specific CD8(+) T cell responses on the single-epitope level over time, starting in primary HIV-1 infection.Methods and findingsWe longitudinally analyzed the polyfunctional epitope-specific CD8(+) T cell responses of 18 patients during primary HIV-1 infection before and after therapy initiation or sequence variation in the targeted epitope. Epitope-specific CD8(+) T cells responded with multiple effector functions to antigenic stimulation during primary HIV-1 infection, but lost their polyfunctional capacity in response to antigen and up-regulated programmed death 1 (PD-1) expression with persistent viremic infection. This exhausted phenotype significantly decreased upon removal of stimulation by antigen, either in response to antiretroviral therapy or by reduction of epitope-specific antigen load in the presence of ongoing viral replication, as a consequence of in vivo selection of cytotoxic T lymphocyte escape mutations in the respective epitopes. Monofunctionality increased in CD8(+) T cell responses directed against conserved epitopes from 49% (95% confidence interval 27%-72%) to 76% (56%-95%) (standard deviation [SD] of the effect size 0.71), while monofunctionality remained stable or slightly decreased for responses directed against escaped epitopes from 61% (47%-75%) to 56% (42%-70%) (SD of the effect size 0.18) (p < 0.05).ConclusionThese data suggest that persistence of antigen can be the cause, rather than the consequence, of the functional impairment of virus-specific T cell responses observed during chronic HIV-1 infection, and underscore the importance of evaluating autologous viral sequences in studies aimed at investigating the relationship between virus-specific immunity and associated pathogenesis.

Published

2008

232. Statistical resolution of ambiguous HLA typing data

Author

Zabrina L. Brumme, Bruce D. Walker, Jennifer Listgarten, Philip J. R. Goulder, Carl M. Kadie, David Heckerman, Mary Carrington, and Gao Xiaojiang

Subjects

Infectious Diseases/Epidemiology and Control of Infectious Diseases, Linkage disequilibrium, Matching (statistics), Immunology, Population, Computational biology, Human leukocyte antigen, Biology, Polymorphism, Single Nucleotide, Sensitivity and Specificity, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Gene Frequency, Genetics, Humans, education, Molecular Biology, Allele frequency, lcsh:QH301-705.5, Alleles, Ecology, Evolution, Behavior and Systematics, Selection (genetic algorithm), 030304 developmental biology, 0303 health sciences, education.field_of_study, HLA-A Antigens, Ecology, Hematology/Bone Marrow and Stem Cell Transplantation, Histocompatibility Testing, Haplotype, Computational Biology, Reproducibility of Results, Genetics and Genomics/Bioinformatics, Infectious Diseases/HIV Infection and AIDS, 3. Good health, Identification (information), Genetics, Population, Haplotypes, Computational Theory and Mathematics, lcsh:Biology (General), Data Interpretation, Statistical, Modeling and Simulation, Genetics and Genomics/Genetics of the Immune System, Algorithms, Research Article, 030215 immunology

Abstract

High-resolution HLA typing plays a central role in many areas of immunology, such as in identifying immunogenetic risk factors for disease, in studying how the genomes of pathogens evolve in response to immune selection pressures, and also in vaccine design, where identification of HLA-restricted epitopes may be used to guide the selection of vaccine immunogens. Perhaps one of the most immediate applications is in direct medical decisions concerning the matching of stem cell transplant donors to unrelated recipients. However, high-resolution HLA typing is frequently unavailable due to its high cost or the inability to re-type historical data. In this paper, we introduce and evaluate a method for statistical, in silico refinement of ambiguous and/or low-resolution HLA data. Our method, which requires an independent, high-resolution training data set drawn from the same population as the data to be refined, uses linkage disequilibrium in HLA haplotypes as well as four-digit allele frequency data to probabilistically refine HLA typings. Central to our approach is the use of haplotype inference. We introduce new methodology to this area, improving upon the Expectation-Maximization (EM)-based approaches currently used within the HLA community. Our improvements are achieved by using a parsimonious parameterization for haplotype distributions and by smoothing the maximum likelihood (ML) solution. These improvements make it possible to scale the refinement to a larger number of alleles and loci in a more computationally efficient and stable manner. We also show how to augment our method in order to incorporate ethnicity information (as HLA allele distributions vary widely according to race/ethnicity as well as geographic area), and demonstrate the potential utility of this experimentally. A tool based on our approach is freely available for research purposes at http://microsoft.com/science., Author Summary At the core of the human adaptive immune response is the train-to-kill mechanism in which specialized immune cells are sensitized to recognize small peptides from foreign sources (e.g., from HIV or bacteria). Following this sensitization, these immune cells are then activated to kill other cells which display this same peptide (and which contain this same foreign peptide). However, in order for sensitization and killing to occur, the foreign peptide must be “paired up” with one of the infected person's other specialized immune molecules—an HLA molecule. The way in which peptides interact with these HLA molecules defines if and how an immune response will be generated. There is a huge repertoire of such HLA molecules, with almost no two people having the same set. Furthermore, a person's HLA type can determine their susceptibility to disease, or the success of a transplant, for example. However, obtaining high quality HLA data for patients is often difficult because of the great cost and specialized laboratories required, or because the data are historical and cannot be retyped with modern methods. Therefore, we introduce a statistical model which can make use of existing high-quality HLA data, to infer higher-quality HLA data from lower-quality data.

Published

2008

233. HIV evolution in response to HLA-restricted CTL selection pressures: a population-based perspective

Author

Jonathan M. Carlson and Zabrina L. Brumme

Subjects

Cellular immunity, Immunology, Population, chemical and pharmacologic phenomena, HIV Infections, Human leukocyte antigen, Microbiology, HLA Antigens, Cytotoxic T cell, Humans, HIV vaccine, Selection, Genetic, education, AIDS Vaccines, education.field_of_study, biology, virus diseases, Genetic Variation, biology.organism_classification, Virology, Biological Evolution, CTL, Infectious Diseases, Genetics, Population, Viral evolution, Lentivirus, HIV-1, T-Lymphocytes, Cytotoxic

Abstract

Cytotoxic T lymphocytes (CTL) recognize antigenic peptides displayed by HLA class I molecules on the infected cell surface and represent a major selective force driving HIV evolution through a phenomenon known as "immune escape". Here we summarize recent advances in our understanding of the consequences of CTL escape on HIV evolution at the population level and discuss its implications for HIV vaccine design.

Published

2008

234. A 21-base pair insertion/duplication at codon 69 of the HIV type 1 reverse transcriptase in a patient undergoing multiple nucleoside therapy

Author

Theresa Mo, P. Richard Harrigan, Zabrina L. Brumme, Paula McKenna, Lee T. Bacheler, and Jennifer S. Hirsch

Subjects

Male, Immunology, Molecular Sequence Data, Context (language use), HIV Infections, Biology, Evolution, Molecular, Abacavir, Virology, Drug Resistance, Viral, medicine, Humans, Didanosine, Genetics, Nucleoside analogue, Stavudine, virus diseases, RNA-Directed DNA Polymerase, Nucleotidyltransferase, Reverse transcriptase, Infectious Diseases, Phenotype, Mutation, HIV-1, Mutagenesis, Site-Directed, Reverse Transcriptase Inhibitors, Nucleoside, medicine.drug

Abstract

We describe the selection of a previously unreported 21-base pair insertion following codon 69 of the HIV-1 reverse transcriptase (RT) from a patient undergoing multiple nucleoside analogue therapy. This insertion was a direct duplication of the preceding 21 bases of HIV-RT, and was selected in a background of NRTI-resistance mutations including substitutions at RT codons 41, 67, 184, 210, and 215. Longitudinal genotypic and phenotypic resistance tests performed before and after selection of the insertion suggested that the insertion conferred an additional decrease in susceptibility to some nucleoside analogues, most notably didanosine, stavudine, abacavir, and tenofovir. However, phenotypic analysis of an insertion-containing site-directed mutant constructed in an HIV-1 HXB2 background revealed no direct association between the 21-base pair insertion and decreased susceptibility to NRTIs, suggesting that the insert requires the context of the patients' virus in order to confer resistance. These observations may offer new insight into the relative contribution of HIV-RT codon 69 insertion mutations to antiretroviral resistance.

Published

2007

235. Evidence of Differential HLA Class I-Mediated Viral Evolution in Functional and Accessory/Regulatory Genes of HIV-1

Author

Zabrina L. Brumme, Chanson J. Brumme, David Heckerman, Bette T. Korber, Marcus Daniels, Jonathan Carlson, Carl Kadie, Tanmoy Bhattacharya, Celia Chui, James Szinger, Theresa Mo, Robert S. Hogg, Julio S. G. Montaner, Nicole Frahm, Christian Brander, Bruce D. Walker, and P. Richard Harrigan

Subjects

lcsh:Immunologic diseases. Allergy, lcsh:Biology (General), Virology, Immunology, Genetics, Correction, Parasitology, lcsh:RC581-607, Molecular Biology, Microbiology, lcsh:QH301-705.5

Published

2007

236. Evidence of differential HLA class I-mediated viral evolution in functional and accessory/regulatory genes of HIV-1

Author

Christian Brander, Theresa Mo, Bruce D. Walker, Julio S. G. Montaner, Zabrina L. Brumme, Nicole Frahm, Carl M. Kadie, Celia Chui, David Heckerman, Robert S. Hogg, Bette T. Korber, P. Richard Harrigan, Chanson J. Brumme, Jonathan M. Carlson, James J. Szinger, Marcus Daniels, and Tanmoy Bhattacharya

Subjects

CD4-Positive T-Lymphocytes, Human Immunodeficiency Virus Proteins, Epitopes, T-Lymphocyte, Genes, MHC Class I, Epitope, 0302 clinical medicine, Viral Regulatory and Accessory Proteins, lcsh:QH301-705.5, Phylogeny, Genetics, 0303 health sciences, education.field_of_study, vpr Gene Products, Human Immunodeficiency Virus, 3. Good health, medicine.anatomical_structure, Viral evolution, Viruses, Research Article, Gene Expression Regulation, Viral, lcsh:Immunologic diseases. Allergy, T cell, Population, Molecular Sequence Data, Immunology, Human leukocyte antigen, Biology, Microbiology, Virus, Evolution, Molecular, Minor Histocompatibility Antigens, 03 medical and health sciences, Immune system, Virology, medicine, Humans, Amino Acid Sequence, nef Gene Products, Human Immunodeficiency Virus, Selection, Genetic, education, Molecular Biology, 030304 developmental biology, Polymorphism, Genetic, Histocompatibility Antigens Class I, CD4 Lymphocyte Count, CTL, lcsh:Biology (General), Mutation, HIV-1, Parasitology, lcsh:RC581-607, 030215 immunology

Abstract

Despite the formidable mutational capacity and sequence diversity of HIV-1, evidence suggests that viral evolution in response to specific selective pressures follows generally predictable mutational pathways. Population-based analyses of clinically derived HIV sequences may be used to identify immune escape mutations in viral genes; however, prior attempts to identify such mutations have been complicated by the inability to discriminate active immune selection from virus founder effects. Furthermore, the association between mutations arising under in vivo immune selection and disease progression for highly variable pathogens such as HIV-1 remains incompletely understood. We applied a viral lineage-corrected analytical method to investigate HLA class I-associated sequence imprinting in HIV protease, reverse transcriptase (RT), Vpr, and Nef in a large cohort of chronically infected, antiretrovirally naïve individuals. A total of 478 unique HLA-associated polymorphisms were observed and organized into a series of “escape maps,” which identify known and putative cytotoxic T lymphocyte (CTL) epitopes under selection pressure in vivo. Our data indicate that pathways to immune escape are predictable based on host HLA class I profile, and that epitope anchor residues are not the preferred sites of CTL escape. Results reveal differential contributions of immune imprinting to viral gene diversity, with Nef exhibiting far greater evidence for HLA class I-mediated selection compared to other genes. Moreover, these data reveal a significant, dose-dependent inverse correlation between HLA-associated polymorphisms and HIV disease stage as estimated by CD4+ T cell count. Identification of specific sites and patterns of HLA-associated polymorphisms across HIV protease, RT, Vpr, and Nef illuminates regions of the genes encoding these products under active immune selection pressure in vivo. The high density of HLA-associated polymorphisms in Nef compared to other genes investigated indicates differential HLA class I-driven evolution in different viral genes. The relationship between HLA class I-associated polymorphisms and lower CD4+ cell count suggests that immune escape correlates with disease status, supporting an essential role of maintenance of effective CTL responses in immune control of HIV-1. The design of preventative and therapeutic CTL-based vaccine approaches could incorporate information on predictable escape pathways., Author Summary One of the greatest challenges facing HIV-1 vaccine design today is the formidable capacity of the virus for mutation and adaptation, a characteristic that has contributed to the extensive worldwide genetic variability of HIV-1 strains observed today. On an individual basis, evolutionary selective pressures imposed by each infected person's unique immune response results in the selection and outgrowth of viral “escape” mutants capable of evading immune recognition, while on a population basis, complex evolutionary selective pressures imposed by the highly polymorphic genes of the human immune system shape HIV-1 diversity on a global level. Making sense of the seemingly infinite complexity of HIV immune escape is of paramount importance in our goal of developing a successful HIV vaccine. The current study uses cutting-edge statistical methods to identify specific sites and patterns of human leukocyte antigen (HLA) class I-restricted escape mutations in various HIV genes. Researchers summarize their findings in the form of “immune escape maps,” which highlight the differential contribution of immune imprinting to HIV genetic diversity, as well as identify specific sites in the viral genome under active immune selection pressure. Results from the present study contribute to our understanding of how human immune selective pressure contributes to variation in different HIV genes, and could help inform the development of HIV vaccines that take into consideration viral diversity.

Published

2007

237. Modest Attenuation of HIV-1 Vpu Alleles Derived from Elite Controller Plasma

Author

Zabrina L. Brumme, Frank Kirchhoff, Oliver T. Fackler, Birthe Mueller, Galit Alter, Johanna Galaski, Nadine Tibroni, Daniel Sauter, Claudia Haller, Takamasa Ueno, Jingyan Chen, Toshiyuki Miura, and Bruce D. Walker

Subjects

Intrinsic immunity, Green Fluorescent Proteins, Human Immunodeficiency Virus Proteins, Molecular Sequence Data, Down-Regulation, lcsh:Medicine, HIV Infections, Virus, Conserved sequence, Immune system, Sequence Analysis, Protein, MHC class I, Humans, Viral Regulatory and Accessory Proteins, Amino Acid Sequence, Receptor, lcsh:Science, Alleles, Conserved Sequence, Phylogeny, Likelihood Functions, Multidisciplinary, biology, Cell Membrane, Histocompatibility Antigens Class I, lcsh:R, NF-kappa B, virus diseases, Virology, HEK293 Cells, Immunology, CD4 Antigens, Tetherin, biology.protein, Disease Progression, HIV-1, RNA, Viral, lcsh:Q, Signal Transduction, Research Article

Abstract

In the absence of antiretroviral therapy, infection with human immunodeficiency virus type 1 (HIV-1) can typically not be controlled by the infected host and results in the development of acquired immunodeficiency. In rare cases, however, patients spontaneously control HIV-1 replication. Mechanisms by which such elite controllers (ECs) achieve control of HIV-1 replication include particularly efficient immune responses as well as reduced fitness of the specific virus strains. To address whether polymorphisms in the accessory HIV-1 protein Vpu are associated with EC status we functionally analyzed a panel of plasma-derived vpu alleles from 15 EC and 16 chronic progressor (CP) patients. Antagonism of the HIV particle release restriction by the intrinsic immunity factor CD317/tetherin was well conserved among EC and CP Vpu alleles, underscoring the selective advantage of this Vpu function in HIV-1 infected individuals. In contrast, interference with CD317/tetherin induced NF-eκB activation was little conserved in both groups. EC Vpus more frequently displayed reduced ability to downregulate cell surface levels of CD4 and MHC class I (MHC-I) molecules as well as of the NK cell ligand NTB-A. Polymorphisms potentially associated with high affinity interactions of the inhibitory killer immunoglobulin-like receptor (KIR) KIR2DL2 were significantly enriched among EC Vpus but did not account for these functional differences. Together these results suggest that in a subgroup of EC patients, some Vpu functions are modestly reduced, possibly as a result of host selection., PLOS ONE, 10(3), e0120434; 2015

Published

2015

238. Effects of human leukocyte antigen class I genetic parameters on clinical outcomes and survival after initiation of highly active antiretroviral therapy

Author

Julio S. G. Montaner, Theresa Mo, Conan K. Woods, Zabrina L. Brumme, P. Richard Harrigan, Chanson J. Brumme, Celia Chui, Bethany M. Henrick, Robert S. Hogg, and Brian Wynhoven

Subjects

Adult, Male, HIV Infections, Disease, Human leukocyte antigen, Cohort Studies, HLA Antigens, Antiretroviral Therapy, Highly Active, Genotype, Immunology and Allergy, Medicine, Humans, Allele, Proportional Hazards Models, Univariate analysis, business.industry, Histocompatibility Testing, Viral Load, Antiretroviral therapy, Survival Analysis, Infectious Diseases, Treatment Outcome, Cohort, Immunology, Multivariate Analysis, HIV-1, RNA, Viral, Female, business, Viral load

Abstract

Human leukocyte antigen (HLA) class I variation influences the progression of untreated human immunodeficiency virus (HIV) disease; however, it is not known whether HLA class I variation may influence clinical outcomes after initiation of highly active antiretroviral therapy (HAART).Associations between HLA class I genotypes and pretherapy clinical parameters were investigated in a cohort of 765 antiretroviral-naive adults initiating HAART. Cox proportional hazards regression was used to investigate the effects of HLA class I genotypes on time to suppression of the viral load to500 HIV RNA copies/mL, time to an increase in the CD4 cell count to100 cells/mm(3) above the baseline count, and time to nonaccidental death over a5-year period after initiation of HAART.Homozygosity at any HLA class I locus and possession of common HLA alleles were associated with a higher pretherapy viral load (P.05). In multivariate analyses controlling for sociodemographic and clinical parameters at baseline, HLA class I homozygosity was significantly associated with a poorer CD4 cell response (P=.008), whereas possession of uncommon HLA alleles was associated with slower virologic suppression after initiation of HAART (P=.02). We observed no significant association between HLA parameters and time to nonaccidental death after initiation of HAART (P.05, univariate analysis).HLA class I zygosity-dependent and frequency-dependent effects may influence short-term HAART outcomes, and, thus, they deserve further investigation. No effects of these HLA parameters on survival after initiation of HAART were observed.

Published

2006

239. The impact of human genetic variation on HIV disease in the era of HAART

Author

Zabrina L, Brumme and P Richard, Harrigan

Subjects

Antiretroviral Therapy, Highly Active, HIV-1, Genetic Variation, Humans, Proteins, HIV Infections, Receptors, Chemokine, Polymorphism, Single Nucleotide

Abstract

Human genetic variation may directly or indirectly influence response to modern antiretroviral therapies for HIV. It is already known that some immunogenetic and other human genetic variations affect the natural history of HIV disease progression where individuals are untreated, but less information is available as to whether these differences are still relevant in the context of HAART. Antiretroviral therapy adds additional opportunities for human genetic contributions to affect variable prognosis--in particular for those genes which influence pharmacokinetics and/or adverse events. To date, the majority of studies investigating the influence of human genetic variation on HIV disease and treatment outcome have focused on single nucleotide polymorphisms or a small number of polymorphisms within a single gene. Reports to date have generally described small effect sizes, and have often been contradictory. Thus, while simple genetic markers relevant to HIV disease or treatment response have indeed been identified (e.g. CCR5delta32 in the context of untreated HIV disease, or HLA-B*5701 allele on the abacavir hypersensitivity reaction in the context of HAART), it is more likely that HIV disease and treatment outcomes are influenced by a multitude of interacting genotypes and phenotypes, a hypothesis that will become increasingly possible to investigate as improvements in molecular and computational technologies are made.

Published

2006

240. HIV VprR77Q mutation does not influence clinical response of individuals initiating highly active antiretroviral therapy

Author

Celia, Chui, Peter K, Cheung, Chanson J, Brumme, Theresa, Mo, Zabrina L, Brumme, Julio S G, Montaner, Andrew D, Badley, and P Richard, Harrigan

Subjects

Adult, Male, Analysis of Variance, British Columbia, Anti-HIV Agents, Genes, vpr, HIV Infections, Viral Load, Article, HIV Long-Term Survivors, Cross-Sectional Studies, Antiretroviral Therapy, Highly Active, Mutation, Disease Progression, HIV-1, Humans, Female

Abstract

VprR77Q has been associated with long-term nonprogressive (LTNP) HIV infection. We wished to investigate the prevalence, clinical correlates, and effect on treatment response of VprR77Q in a cohort of antiretroviral-naïve individuals initiating Highly Active Antiretroviral Therapy (HAART). Baseline plasma samples from 728 subjects were genotyped using RT-PCR and direct DNA sequencing. Cox proportional hazards regression was used to model the effects of VprR77Q on virologic and immunologic responses, and survival following initiation of HAART, over a median 4.5 years follow-up. We found that 308 subjects (42.3%) harbored VprR77Q alone or in combination with another amino acid, while 420 (57.7%) harbored an amino acid other than Q. A cross-sectional analysis found no correlation between R77Q and baseline plasma viral load (pVL), CD4 count, diagnosis of AIDS, or sociodemographic characteristics including age, gender and history of injection drug use (p > 0.1). In multivariate analyses, no significant associations between VprR77Q and initial pVL and CD4 responses to HAART (p > 0.1) or survival following initiation of treatment were observed. The high prevalence and the lack of association with pre-therapy clinical parameters in this cohort argue against an association of R77Q with LTNP status. These results do not support an association between R77Q and HAART response.

Published

2006

241. Short communication. Association of the CCR5delta32 mutation with clinical response and5-year survival following initiation of first triple antiretroviral regimen

Author

Zabrina L, Brumme, Bethany M, Henrick, Chanson J, Brumme, Robert S, Hogg, Julio S G, Montaner, and P Richard, Harrigan

Subjects

Adult, Male, Time Factors, Genotype, Receptors, CCR5, Anti-HIV Agents, HIV Infections, Viral Load, Prognosis, Survival Rate, Treatment Outcome, Risk Factors, Antiretroviral Therapy, Highly Active, Mutation, Disease Progression, Humans, Female, Prospective Studies, Proportional Hazards Models

Abstract

The CCR5delta32 mutation is associated with slower HIV disease progression in untreated infection. However, it remains controversial as to whether CCR5delta32 is a relevant prognostic marker in the context of highly active antiretroviral therapy (HAART). Here we investigate associations between CCR5delta32 and HAART outcomes in a large, population-based cohort of1000 antiretroviral-naive individuals initiating triple therapy over a median5 year follow-up.CCR5delta32 genotypes were determined using PCR and DNA sequencing in a cohort of 1188 antiretroviral-naive individuals initiating triple therapy in British Columbia. Associations between CCR5delta32 and baseline (pre-therapy) sociodemographic and clinical parameters were investigated in a cross-sectional analysis. Cox proportional hazards regression was used to investigate the effect of CCR5delta32 on clinical outcomes following therapy initiation. The endpoints that were evaluated included time to plasma viral load (pVL) suppression400 copies HIV RNA/ml, subsequent time to pVL reboundor =400 copies/ml, time to CD4+ cell decline below baseline, and time to non-accidental death over a median5 year follow-up.CCR5delta32 genotypes were available for 1174 of 1188 individuals (98.8%): 171 (14.6%) CCR5wt/delta32 and 1003 (85.4%) CCR5wt/wt. At baseline, CCR5wt/delta32 individuals had higher CD4+ cell counts (P=0.04), lower plasma viral loads (P=0.06) and were slightly older than CCR5wt/wt individuals (P=0.04). In multivariate analyses controlling for baseline parameters and adherence estimates, we observed a significant association between CCR5wt/delta32 and a shorter time to initial pVL suppression400 copies/ml (multivariate hazard ratio [HR]: 1.20; 95% confidence interval [CI]: 1.01-1.44). No associations were observed between CCR5delta32 and other clinical outcomes including subsequent time to pVL rebound or time to CD4+ cell decline below baseline. In univariate analyses, we observed a significant association between CCR5wt/delta32 genotype and improved survival over the median5 year period following initiation of HAART (P=0.03). However, this association did not remain significant in multivariate analyses after adjusting for baseline factors including adherence (multivariate HR: 0.64; 95% CI: 0.38-1.07; P=0.09)Results indicate that, after controlling for adherence, the CCR5delta32 mutation is likely not a clinically significant predictor of longer-term clinical responses or survival in the context of HAART.

Published

2005

242. Treatment interruption of highly active antiretroviral therapy in patients with nadir CD4 cell counts200 cells/mm3

Author

Zabrina L. Brumme, Marianne Harris, Richard Harrigan, Julio S. G. Montaner, Adrienne R. Toulson, Katherine V. Heath, Robert S. Hogg, and Benita Yip

Subjects

Adult, Male, medicine.medical_specialty, Prognostic variable, HIV Infections, Gastroenterology, Drug Administration Schedule, Acquired immunodeficiency syndrome (AIDS), Internal medicine, Antiretroviral Therapy, Highly Active, Genotype, Immunology and Allergy, Medicine, Humans, Genotyping, Proportional Hazards Models, business.industry, Proportional hazards model, Drug holiday, Middle Aged, medicine.disease, CD4 Lymphocyte Count, Infectious Diseases, Treatment Outcome, Immunology, Multivariate Analysis, HIV-1, Female, business, Viral load, Nadir (topography)

Abstract

The goal of the present study was to characterize outcome and predictors of outcome of treatment interruption (TI) in highly active antiretroviral therapy (HAART)-treated patients.A systematic chart/database review was conducted to identify patients with nadir CD4 cell counts200 cells/mm(3) and without acquired immunodeficiency syndrome-defining illnesses who underwent a TI. Collected data included duration and reason for TI, demographic characteristics, CD4 cell count, and plasma viral load. Human immunodeficiency virus (HIV) envelope (V3) loop genotyping was performed on plasma HIV RNA. The presence of basic residues at aa 11 and/or 25 (the "11/25" genotype) was a further possible prognostic variable of interest. Cox proportional hazards models were used to assess characteristics associated with time to HAART reinitiation after TI.A total of 208 of 4461 (4.7%) patients underwent TI. The study group consisted of 197 (94.7%) of 208 participants for whom V3 genotyping was successful. The median CD4 cell count at time of the initiation of TI was 620 cells/mm(3). A total of 59 (29.9%) patients reinitiated HAART after a median of 15 months. At the time of the reinitiation of HAART, the median plasma viral load was100,000 copies/mL, and the median CD4 cell count was 260 cells/mm(3). Among the 197 study patients, there were 6 deaths, none of which was attributable to the TI. A total of 81% had plasma viral loads50 copies/mL by 15 months of follow-up after reinitiation of HAART. In multivariate analysis, a nadir CD4 cell countor =250 cells/mm(3) (risk ratio [RR], 2.79 [95% confidence interval [CI], 1.60-4.86]; P.001) and the presence of the 11/25 genotype (RR, 2.07 [95% CI, 1.07-4.02]; P = .031) were positively and independently associated with faster time to HAART reinitiation, after adjusting for age and plasma virus load at the start of TI.Our study suggests that TI is a viable option for HIV-positive adults with nadir CD4 cell counts250 cells/mm(3). A nadir CD4 cell count of 200-250 cells/mm(3) and the 11/25 viral genotype were found to be associated with a faster HAART reinitiation.

Published

2005

243. Molecular and clinical epidemiology of CXCR4-using HIV-1 in a large population of antiretroviral-naive individuals

Author

Zabrina L. Brumme, Peter K. Cheung, Julio S. G. Montaner, P. Richard Harrigan, Chanson J. Brumme, Robert S. Hogg, James Goodrich, Jerome J. Asselin, Brian Wynhoven, Bethany M. Henrick, and Howard Mayer

Subjects

Adult, Male, medicine.medical_specialty, Receptors, CXCR4, Multivariate analysis, Genotype, Anti-HIV Agents, Population, HIV Infections, V3 loop, Epidemiology, HIV tropism, medicine, Immunology and Allergy, Humans, education, education.field_of_study, Analysis of Variance, Molecular Epidemiology, biology, British Columbia, Genetic Variation, Middle Aged, biology.organism_classification, CD4 Lymphocyte Count, Infectious Diseases, Phenotype, Treatment Outcome, Lentivirus, Immunology, Multivariate Analysis, HIV-1, Female, Panton–Valentine leukocidin

Abstract

OBJECTIVE We wished to characterize the epidemiological and clinical correlates of CXCR4-using human immunodeficiency virus type 1 (HIV-1) ("X4 variants") in a cross-sectional analysis of a large population of antiretroviral-naive individuals. METHODS HIV-1 coreceptor use was determined in the last pretherapy plasma sample for 1191 individuals initiating triple-combination therapy in British Columbia, Canada. Baseline variables investigated included sociodemographic characteristics, plasma viral load (pVL), CD4 cell count, AIDS diagnosis, HIV-1 V3 loop sequence, and human CCR5 Delta 32 genotype. RESULTS Individuals harboring X4 variants (n = 178 of 979 phenotyped samples; 18.2%) displayed a poorer baseline clinical profile than individuals harboring exclusively CCR5-using HIV-1 ("R5 variants") (median pVL, 175,000 vs. 120,000 copies of HIV-1 RNA/mL [P = .0006]; median CD4 cell count, 110 vs. 290 cells/mm(3) [P < .0001]). Individuals heterozygous for the CCR5 Delta 32 deletion (n = 128 of 967; 13.2%) were at 2.5 times higher risk of harboring X4 variants, compared with those without the deletion (multivariate P = .0005). The presence of basic amino acids at codon 11 and/or codon 25 of HIV-1 V3 (n = 109 of 955; 11.4%) was associated with a 9.1 times higher risk of harboring X4 variants (multivariate P < .0001), regardless of CCR5 Delta 32 genotype. In multivariate analyses adjusting for baseline parameters, HIV-1 coreceptor use was not found to be a significant predictor of survival or treatment response. CONCLUSION Baseline CD4 cell count, pVL, HIV-1 V3 sequence, and CCR5 Delta 32 genotype were the strongest determinants of CXCR4-using HIV-1 in this population. After adjustment for baseline parameters, the presence of X4 variants before initiation of highly active antiretroviral therapy was not independently associated with a poorer outcome of therapy.

Published

2004

244. Clinical and immunological impact of HIV envelope V3 sequence variation after starting initial triple antiretroviral therapy

Author

Zabrina L. Brumme, Robert S. Hogg, Julio S. G. Montaner, James I. Mullins, Brian Wynhoven, Noah G. Hoffman, Benita Yip, Mark A. Jensen, Winnie Dong, Ronald Swanstrom, and P. Richard Harrigan

Subjects

Adult, Male, Genotype, Immunology, HIV Infections, Drug resistance, V3 loop, HIV Envelope Protein gp120, Cohort Studies, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, Immunology and Allergy, Medicine, Humans, Risk factor, Survival analysis, biology, business.industry, Genetic Variation, Viral Load, biology.organism_classification, Prognosis, Virology, Survival Analysis, Peptide Fragments, CD4 Lymphocyte Count, Infectious Diseases, Phenotype, Treatment Outcome, Lentivirus, HIV-1, Female, Viral disease, Neural Networks, Computer, business, Viral load

Abstract

BACKGROUND: The HIV-1 envelope third variable loop (V3 loop) is an important determinant of viral phenotype and co-receptor usage. We wished to determine the impact of specific V3 genotypes associated with viral phenotype and co-receptor usage on response to initial triple antiretroviral therapy. METHODS: Pre-therapy plasma samples from the HOMER cohort of 1191 antiretroviral-naive, HIV-infected adults who initiated triple therapy in British Columbia, Canada between August 1996 and September 1999 were genotyped for V3 loop sequence. V3 sequences were dichotomized by the presence or absence of positively charged residues at codons 11 and/or 25 (an '11/25' genotype). Neural network (NN) and Position Specific Scoring Matrix (PSSM) approaches were used as alternative V3 sequence interpretation methods. The association of V3 genotypes with clinical endpoints was assessed over a median of 43 months of follow up. RESULTS: One-hundred and eighteen (10.9%) of the 1085 isolates successfully genotyped for V3 displayed the 11/25 genotype. In multivariate analyses, this genotype was associated with a more rapid CD4 decline [risk ratio, (RR), 1.38; P = 0.012] and earlier mortality (RR, 1.70; P = 0.027), despite comparable viral load suppression below 500 HIV RNA copies/ml. We observed no influence of the 11/25 genotype on time to viral rebound or the development of drug resistance. PSSM-based sequence categories were similarly predictive of outcomes. NN sequence categories were not associated with any endpoints. CONCLUSION: The 11/25 genotype of the HIV V3 loop is an independent predictor of poor immunological response and more rapid mortality even after starting triple antiretroviral therapy. These results may prove to be useful for the clinical management of HIV-infected individuals.

Published

2004

245. Prevalence and clinical implications of insertions in the HIV-1 p6Gag N-terminal region in drug-naive individuals initiating antiretroviral therapy

Author

Zabrina L, Brumme, Keith J, Chan, Winnie W Y, Dong, Brian, Wynhoven, Theresa, Mo, Robert S, Hogg, Julio S G, Montaner, Michael V, O'Shaughnessy, and P Richard, Harrigan

Subjects

Adult, Male, British Columbia, Genotype, Anti-HIV Agents, Gene Products, gag, HIV Infections, HIV Envelope Protein gp120, Viral Load, Survival Analysis, gag Gene Products, Human Immunodeficiency Virus, Peptide Fragments, CD4 Lymphocyte Count, Cohort Studies, Mutagenesis, Insertional, Drug Resistance, Viral, HIV-1, Prevalence, Humans, Female, Proportional Hazards Models

Abstract

We assessed the prevalence and clinical impact of insertions within the HIV-1 p6Gag proline-rich (PTAP) region on initial antiretroviral therapy response in 461 HIV-infected, drug-naive individuals initiating therapy in British Columbia, Canada between June 1996 and August 1998. HIV p6Gag insertions were detected by nested RT-PCR of extracted patient plasma followed by direct DNA sequencing. Insertions were observed in 70 of 423 successfully genotyped samples (16.5%). HIV p6Gag insertions were significantly associated with a lower baseline CD4 cell count (P0.05) and the presence of basic amino acids at key positions in the HIV envelope V3 loop linked to a syncytium-inducing phenotype (P0.05). After adjusting for baseline factors, no effect of HIV p6Gag insertions was observed on time to virological success (pVLor = 500 copies/ml), virological failure (subsequent confirmed pVLor = 500 copies/ml) or immunological failure (confirmed CD4 count below baseline), as evaluated by Kaplan-Meier methods and Cox proportional hazard regression (P0.1). The data suggest that HIV p6Gag insertions are not exclusively related to drug resistance and may not influence response to antiretroviral therapy, but may be linked to sequence variations in the HIV envelope.

Published

2003

246. No association between GB virus-C viremia and virological or immunological failure after starting initial antiretroviral therapy

Author

P. Richard Harrigan, Michael V. O'Shaughnessy, Winnie Dong, Keith Chan, Julio S. G. Montaner, Robert S. Hogg, Zabrina L. Brumme, Brian Wynhoven, and Theresa Mo

Subjects

Adult, Male, Hepatitis, Viral, Human, Anti-HIV Agents, Immunology, Population, Viremia, GB virus C, HIV Infections, Virus, Cohort Studies, Flaviviridae, Plasma, Acquired immunodeficiency syndrome (AIDS), Antiretroviral Therapy, Highly Active, medicine, Immunology and Allergy, Humans, education, Proportional Hazards Models, education.field_of_study, biology, Proportional hazards model, business.industry, Reverse Transcriptase Polymerase Chain Reaction, HIV, Flaviviridae Infections, Viral Load, biology.organism_classification, medicine.disease, Virology, CD4 Lymphocyte Count, Infectious Diseases, RNA, Viral, Female, Viral disease, business

Abstract

Introduction: Co-infection with GBV-C (`Hepatitis G’ virus) appears to be associated with slower disease progression in HIV-infected, untreated individuals. We wished to determine whether detection of GBV-C RNA was associated with differential response to HIV therapy in a population-based cohort of 461 individuals initiating antiretroviral therapy between June 1996 and August 1998, in British Columbia, Canada. Methods: The presence of GBV-C RNA in plasma was identified by nested RT–PCR, using detection of HIV gag RNA as a positive control. Time to virological success [achieving HIV plasma viral load (pVL) ≤ 500 copies/ml], virological failure (subsequent confirmed pVL > 500 copies/ml) and immunological failure (confirmed CD4 cell count below baseline) were assessed by Kaplan–Meier methods and Cox proportional hazard regression. Results: Of the 441 individuals for whom results were available, 90 (20.4%) had detectable plasma GBV-C RNA. GBV-C RNA was significantly associated with a lower HIV pVL at baseline (P = 0.004). In univariate and multivariate Cox models, GBV-C RNA positive and negative individuals did not differ with respect to time to virological success [risk ratio (RR), 0.98; 95% confidence interval (CI), 0.75–1.27], time to virological failure (RR, 1.10; 95% CI, 0.74–1.65), or time to immunological failure (RR, 1.09; 95% CI, 0.73–1.63). There was no correlation between detection of GBV-C RNA and mutations in the human chemokine receptors CCR5 and CX3CR1, or HIV viral tropism as predicted by the HIV envelope sequence (P > 0.1). Conclusion: GBV-C viremia is relatively common in individuals seeking treatment for HIV infection; however, it does not appear to have any effect on initial antiretroviral therapy response.

Published

2002

247. A Mutation in the 3′ Region of the Human Immunodeficiency Virus Type 1 Reverse Transcriptase (Y318F) Associated with Nonnucleoside Reverse Transcriptase Inhibitor Resistance

Author

Zabrina L. Brumme, P. Richard Harrigan, Brian Wynhoven, Brendan Larder, Paula McKenna, Mahboob Salim, David K. Stammers, and S. D. Kemp

Subjects

Models, Molecular, Efavirenz, Nevirapine, Anti-HIV Agents, Immunology, Mutant, Drug resistance, Microbial Sensitivity Tests, Biology, medicine.disease_cause, Microbiology, chemistry.chemical_compound, Virology, Vaccines and Antiviral Agents, Drug Resistance, Viral, medicine, Delavirdine, Humans, 3' Untranslated Regions, Mutation, Reverse-transcriptase inhibitor, virus diseases, Reverse transcriptase, HIV Reverse Transcriptase, chemistry, Insect Science, HIV-1, Mutagenesis, Site-Directed, Reverse Transcriptase Inhibitors, medicine.drug

Abstract

The Y318F substitution in the 3′ region of human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) has been linked to nonnucleoside RT inhibitor (NNRTI) resistance in vitro. A systematic search of a large phenotypic-genotypic database (Virco) linked the Y318F substitution with a >10-fold decrease in NNRTI susceptibility in >85% of clinically derived isolates. There was a significant association between Y318F and use of delavirdine ( P = 10 −11 ) and nevirapine ( P = 10 −6 ) but not efavirenz ( P = 0.3). Site-directed HIV-1 Y318F mutants in an HXB2 background displayed 42-fold-decreased susceptibility to delavirdine but 100- and >60-fold decreases in delavirdine and nevirapine susceptibility, respectively. These results indicate the importance of the Y318F substitution in HIV-1 drug resistance.

Published

2002

248. Changes in mitochondrial DNA as a marker of nucleoside toxicity in HIV-infected patients

Author

Lillian Ting, Zabrina L. Brumme, Kevin J. P. Craib, Marianne Harris, Christopher S. Alexander, Michael V. O'Shaughnessy, Julio S. G. Montaner, P. Richard Harrigan, Hélène C. F. Côté, Hubert Wong, and Brian Wynhoven

Subjects

Adult, Genetic Markers, Male, Mitochondrial DNA, Drug-Related Side Effects and Adverse Reactions, Anti-HIV Agents, HIV Infections, DNA, Mitochondrial, Polymerase Chain Reaction, Virus, law.invention, law, Medicine, Humans, Lactic Acid, Longitudinal Studies, Polymerase chain reaction, Polymerase, biology, business.industry, General Medicine, DNA, Middle Aged, medicine.disease, Virology, Dideoxynucleosides, Nuclear DNA, Lactic acidosis, biology.protein, Hyperlactatemia, Drug Therapy, Combination, business, Nucleoside

Abstract

Nucleoside analogues can induce toxic effects on mitochondria by inhibiting the human DNA polymerase gamma. The toxic effects can range from increased serum lactate levels to potentially fatal lactic acidosis. We studied changes in mitochondrial DNA relative to nuclear DNA in the peripheral-blood cells of patients with symptomatic, nucleoside-induced hyperlactatemia.Total DNA was extracted from blood cells. A nuclear gene and a mitochondrial gene were quantified by real-time polymerase chain reaction. Three groups were studied: 24 controls not infected with the human immunodeficiency virus (HIV), 47 HIV-infected asymptomatic patients who had never been treated with antiretroviral drugs, and 8 HIV-infected patients who were receiving antiretroviral drugs and had symptomatic hyperlactatemia. The patients in the last group were studied longitudinally before, during, and after antiretroviral therapy.Symptomatic hyperlactatemia was associated with marked reductions in the ratios of mitochondrial to nuclear DNA, which, during therapy, averaged 68 percent lower than those of non-HIV-infected controls and 43 percent lower than those of HIV-infected asymptomatic patients never treated with antiretroviral drugs. After the discontinuation of antiretroviral therapy, there was a statistically significant increase in the ratio of mitochondrial to nuclear DNA (P=0.02). In the patients followed longitudinally, the decline in mitochondrial DNA preceded the increase in venous lactate levels.Mitochondrial DNA levels are significantly decreased in patients with symptomatic, nucleoside-related hyperlactatemia, an effect that resolves on the discontinuation of therapy.

Published

2002

249. Transmitted Escape Mutations Lead to Accelerated HIV-1 Disease Progression and Largely Define the Relative Contribution of HLA Alleles to Control

Author

Eric Hunter, Simon Mallal, Zabrina L. Brumme, Chanson J. Brumme, Malinda Schaefer, Jonathan M. Carlson, Roger L. Shapiro, Mina John, Nico Pfeifer, David Heckerman, Philip J. R. Goulder, Thumbi Ndung'u, and John Frater

Subjects

Infectious Diseases, Virology, Immunology, Disease progression, Human immunodeficiency virus (HIV), medicine, Human leukocyte antigen, Biology, Allele, medicine.disease_cause

Published

2014

250. Reply to Waters et al

Author

P. Richard Harrigan, Chanson J. Brumme, Zabrina L. Brumme, and Celia Chui

Subjects

Microbiology (medical), Infectious Diseases, Oceanography, business.industry, Medicine, business

Published

2007