Your search keyword '"Bette T. Korber"' showing total 18 results

1. T Cell Responses in HIV Type 1-Infected Adolescent Minorities Share Similar Epitope Specificities with Whites Despite Significant Differences in HLA Class I Alleles

Author

Christopher Perkins, Bradley H. Edwards, Steffanie Sabbaj, Paul A. Goepfert, Doug Ritter, James Tang, Richard A. Kaslow, James J. Szinger, Bette T. Korber, Mark J. Mulligan, Heidi L. Weiss, Anju Bansal, and Craig M. Wilson

Subjects

Adult, Cellular immunity, Adolescent, Anti-HIV Agents, T-Lymphocytes, viruses, T cell, Molecular Sequence Data, Immunology, Population, Retroviridae Proteins, Black People, Epitopes, T-Lymphocyte, HIV Infections, Human leukocyte antigen, Biology, White People, Epitope, Virology, Immunopathology, Genetic variation, medicine, Humans, Amino Acid Sequence, Allele, education, Alleles, Genetics, education.field_of_study, Histocompatibility Testing, Histocompatibility Antigens Class I, Hispanic or Latino, Infectious Diseases, medicine.anatomical_structure, HIV-1, Female, Peptides, Epitope Mapping

Abstract

African-Americans (AFAM) and Hispanics (HIS) represent only 13% and 12% of the U.S. population but 54% and 19%, respectively, of annually incident HIV-1 infections in the United States. The 88 patients in the current study were from U.S. racial or ethnic minority groups (72% African-American, 17% Hispanic), female (85%), and adolescent (mean age 20 years). Their HLA allele distributions were distinct from patterns in U.S. whites. Overall, HIV-1-specific T cell responses were observed in 91% of participants: 75% recognized peptides in Gag, 67% Pol, 57% Nef, and 41% Env. The patients recognized 87 (36%) of 244 Gag, Pol, Env, or Nef peptides tested. Similar to what has been seen in white cohorts, epitope-rich peptide clusters were identified within conserved functional domains in Gag matrix, Gag capsid, Pol reverse transcriptase, and Nef. Peptides representing variable regions from within the B subtype or with more changes from the B subtype consensus sequence were less likely to stimulate a positive T cell response. A small percentage (17%) of unique T cell responses was found in this cohort that displayed no previously known T cell epitopes. Dominant responses generally overlapped with epitope-rich regions in HIV-1 described previously for whites, although many of these peptides were likely restricted by HLA class I alleles not previously associated with these epitopes. Hence host genetic variation among different racial groups may have less impact on the utility of candidate HIV-1 vaccines than previously suspected.

Published

2003

2. Identification of a Novel Clade of Human Immunodeficiency Virus Type 1 in Democratic Republic of Congo

Author

Jean K. Carr, Deborah L. Birx, John L. Mokili, Peter Simmonds, Bette T. Korber, Brian T. Foley, Melissa Rogers, Johnny M. Bopopi, and Francine E. McCutchan

Subjects

Genetics, education.field_of_study, Lineage (genetic), Phylogenetic tree, Genetic heterogeneity, Immunology, Population, Biology, Genome, Virology, Infectious Diseases, Phylogenetics, Genotype, Democratic Republic of the Congo, HIV-1, Humans, Amino Acid Sequence, Clade, education, Phylogeny

Abstract

The high genetic heterogeneity of HIV-1 in the Democratic Republic of Congo (DRC) constitutes a real challenge for the development of vaccines to counter the spread of the HIV-1 epidemic. It is important to continue to monitor the epidemic by studying the circulating strains and their impact on the overall spread. As part of the ongoing effort to study the global distribution of HIV-1 subtypes and circulating recombinant forms (CRFs), here we describe a new phylogenetic clade of HIV-1 by the analysis of two full-length sequences (83CD003 and 90CD121E12) collected from two individuals at a 7-year interval (1983 and 1990, respectively). One of the two sequences (90CD121E12) was obtained from a vertically infected, 12-month-old baby in Kimpese, rural DRC, an area with low and stable seroprevalence of HIV-1 in women attending antenatal clinics. The two sequences are genetically similar by 95% of their full genome and topologically form a distinct cluster that is equidistant from the existing subtypes (A through K) by the analysis of both the full genome and subgenomic regions. Furthermore, they share several other genetic features, including an additional pair of cysteine residues, predictive of an extra disulfide bridge, in the V4 loop of gp120. This new clade is currently rare, spreading at a slower pace than the other subtypes found in the DRC region. Pending the identification of at least one partial length sequence of the same lineage from another patient who is epidemiologically unlinked to those described here, this clade is not yet named as a subtype as per the recommendation of the nomenclature committee.

Published

2002

3. Molecular Characterization of a Highly Divergent HIV Type 1 Isolate Obtained Early in the AIDS Epidemic from the Democratic Republic of Congo

Author

Stanley A. Trask, Bette T. Korber, Beatrice H. Hahn, George M. Shaw, Yalu Chen, Feng Gao, Olga Mamaeva, Theodore S. Theodore, Huxong Hui, and Brian T. Foley

Subjects

Lineage (genetic), Phylogenetic tree, Sequence analysis, Molecular Sequence Data, Immunology, HIV Infections, Genome, Viral, Sequence Analysis, DNA, Biology, Transfection, Virology, Genome, Virus, Cell Line, Disease Outbreaks, Evolution, Molecular, Infectious Diseases, Phylogenetics, Democratic Republic of the Congo, HIV-1, Humans, Viral disease, Gene, Phylogeny

Abstract

Numerous complete human immunodeficiency virus type 1 (HIV-1) genomes have been characterized for contemporary viruses, but few isolates obtained early in the HIV-1 epidemic have been studied. In this article, we describe the molecular characterization of an HIV-1 isolate (83CD003) that was obtained from an AIDS patient in Kinshasa, Democratic Republic of Congo (DRC) in 1983. The complete 83CD003 genome was sequenced in its entirety and found to encode uninterrupted open reading frames for all viral genes. Phylogenetic analysis revealed 83CD003 was a member of the major (M) group of HIV -1, but did not group with any of the known subtypes. Rather, it formed an independent lineage in all regions of its genome that was roughly equidistant from representatives of all other subtypes. Similarly, 83CD003 also did not cluster with any of several unclassified group M sequences that have been reported more recently to circulate in the DRC, suggesting that it may represent an early group M lineage thai is either rare or has gone extinct. The molecular clone of 83CD003 yielded an infectious virus after transfection into mammalian cells and its biological properties can be further studied.

Published

2001

4. The Thai Phase III HIV Type 1 Vaccine trial (RV144) regimen induces antibodies that target conserved regions within the V2 loop of gp120

Author

Nicos, Karasavvas, Erik, Billings, Mangala, Rao, Constance, Williams, Susan, Zolla-Pazner, Robert T, Bailer, Richard A, Koup, Sirinan, Madnote, Duangnapa, Arworn, Xiaoying, Shen, Georgia D, Tomaras, Jeffrey R, Currier, Mike, Jiang, Craig, Magaret, Charla, Andrews, Raphael, Gottardo, Peter, Gilbert, Timothy J, Cardozo, Supachai, Rerks-Ngarm, Sorachai, Nitayaphan, Punnee, Pitisuttithum, Jaranit, Kaewkungwal, Robert, Paris, Kelli, Greene, Hongmei, Gao, Sanjay, Gurunathan, Jim, Tartaglia, Faruk, Sinangil, Bette T, Korber, David C, Montefiori, John R, Mascola, Merlin L, Robb, Barton F, Haynes, Viseth, Ngauy, Nelson L, Michael, Jerome H, Kim, Mark S, de Souza, and Patricia, Morgan

Subjects

Male, Immunology, Molecular Sequence Data, Protein Array Analysis, Epitopes, T-Lymphocyte, Enzyme-Linked Immunosorbent Assay, HIV Infections, Biology, HIV Antibodies, HIV Envelope Protein gp120, Cell Line, Virology, Humans, Amino Acid Sequence, Peptide sequence, AIDS Vaccines, Vaccines, Vaccine trial, Vaccination, Loop (topology), Regimen, Infectious Diseases, AIDSVAX, biology.protein, HIV-1, Female, Peptide microarray, Antibody

Abstract

The Thai Phase III clinical trial (RV144) showed modest efficacy in preventing HIV-1 acquisition. Plasma collected from HIV-1-uninfected trial participants completing all injections with ALVAC-HIV (vCP1521) prime and AIDSVAX B/E boost were tested for antibody responses against HIV-1 gp120 envelope (Env). Peptide microarray analysis from six HIV-1 subtypes and group M consensus showed that vaccination induced antibody responses to the second variable (V2) loop of gp120 of multiple subtypes. We further evaluated V2 responses by ELISA and surface plasmon resonance using cyclic (Cyc) and linear V2 loop peptides. Thirty-one of 32 vaccine recipients tested (97%) had antibody responses against Cyc V2 at 2 weeks postimmunization with a reciprocal geometric mean titer (GMT) of 1100 (range: 200–3200). The frequency of detecting plasma V2 antibodies declined to 19% at 28 weeks post-last injection (GMT: 110, range: 100–200). Antibody responses targeted the mid-region of the V2 loop that contains conserved epitopes and has the amino acid sequence KQKVHALFYKLDIVPI (HXB2 Numbering sequence 169–184). Valine at position 172 was critical for antibody binding. The frequency of V3 responses at 2 weeks postimmunization was modest (18/32, 56%) with a GMT of 185 (range: 100–800). In contrast, naturally infected HIV-1 individuals had a lower frequency of antibody responses to V2 (10/20, 50%; p=0.003) and a higher frequency of responses to V3 (19/20, 95%), with GMTs of 400 (range: 100–3200) and 3570 (range: 200–12,800), respectively. RV144 vaccination induced antibodies that targeted a region of the V2 loop that contains conserved epitopes. Early HIV-1 transmission events involve V2 loop interactions, raising the possibility that anti-V2 antibodies in RV144 may have contributed to viral inhibition.

Published

2012

5. The World Health Organization Global Programme on AIDS Proposal for Standardization of HIV Sequence Nomenclature

Author

José Esparza, Gerald Myers, Bette T. Korber, and Saladin Osmanov

Subjects

Medical education, Standardization, Immunology, Human immunodeficiency virus (HIV), Biology, medicine.disease, medicine.disease_cause, Virology, World health, Infectious Diseases, Acquired immunodeficiency syndrome (AIDS), medicine, Nomenclature

Abstract

The World Health Organization Global Programme on AIDS (WHO/GPA) is conducting a large-scale collaborative study of human immunodeficiency virus type 1 (HIV-1) variation, based in four potential va...

Published

1994

6. Standard Conditions of Virus Isolation Reveal Biological Variability of HIV Type 1 in Different Regions of the World

Author

Björndal A, Etienne Karita, Tomlinson P, Shahin Ranjbar, Esser R, von Briesen H, Harvey Holmes, Bette T. Korber, Bernardo Galvão-Castro, and H. Rübsamen-Waigmann

Subjects

Syncytium, viruses, Immunology, Biology, Virology, Virus, Infectious Diseases, Immune system, Viral replication, Immunity, Genotype, Genetic variation, Seroconversion

Abstract

HIV-1 isolates were obtained from four countries within the framework of the WHO Network for HIV Isolation and Characterization. The use of standard HIV isolation procedures allowed us to compare the biological properties of 126 HIV-1 isolates spanning five genetic subtypes. In primary isolation cultures, viruses from Uganda and Brazil appeared early and replicated without delay, whereas the replication of Thai viruses was delayed by several weeks. Regardless of genetic subtype or country of origin, blood samples collected more than 2 years after seroconversion yielded virus that replicated efficiently in the primary isolation cultures. None of the isolates obtained from Thailand or Rwanda replicated in cell lines, whereas 5 of the 13 Brazilian isolates and 7 of the 11 Ugandan isolates replicated and induced syncytia in MT-2 cells. As expected for virus isolates obtained early in HIV-1 infection (within 2 years of seroconversion), all viruses from Brazil, Rwanda, and Thailand showed a slow/low replicative pattern. For the Ugandan samples, the time from seroconversion was known precisely for a few of the samples and only in one case was less than 2 years. This may explain why the five viruses that were able to replicate in all cell lines, and thus classified as rapid/high, were of Ugandan origin. Viruses able to induce syncytia in MT-2 cells, also induced syncytia in PBMC. However, 8 slow/low viruses (out of 27) gave discordant results, inducing syncytia in PBMC but not in MT-2 cells. Furthermore, using syncytium induction as a marker, changes in virus populations during early in vitro passage in PBMC could be observed

Published

1994

7. AIDS research pioneer Gerry Myers dies

Author

Brian T. Foley and Bette T. Korber

Subjects

Acquired Immunodeficiency Syndrome, Infectious Diseases, Virology, Immunology, Genetic Variation, HIV, Humans, History, 20th Century, History, 21st Century

Published

2011

8. Signature Pattern Analysis: A Method for Assessing Viral Sequence Relatedness

Author

Bette T. Korber and Gerald Myers

Subjects

Male, Dentists, Molecular Sequence Data, Immunology, Mothers, HIV Infections, Sequence alignment, Computational biology, Biology, Cohort Studies, Set (abstract data type), Sequence Homology, Nucleic Acid, Virology, Genetic variation, Humans, Amino Acid Sequence, Peptide sequence, Genetics, Linkage (software), Base Sequence, Sequence Homology, Amino Acid, Nucleic acid sequence, Genetic Variation, Phenotype, Signature (logic), Sexual Partners, Infectious Diseases, HIV-1, Female, Sequence Alignment

Abstract

Signature pattern analysis identifies particular sites in amino acid or nucleic acid alignments of variable sequences that are distinctly representative of a query set of sequences relative to a background set. We explore the merits of using signature patterns for analysis of HIV-1 (human immunodeficiency virus type 1) sequences in cases of epidemiological linkage and potential superinfection. For these purposes, query sets are viral sequences that are all derived from one HIV-1 infected individual, hence the signature pattern is the array of sites that are characteristic of the range of viral variants obtained from that person. Once a signature pattern has been objectively defined, it can be used to examine other viral sequences from other individuals for evidence of genetic relatedness. A computer program to facilitate this analysis, VESPA, is described and applied to sequence data gathered during the investigation of HIV-1 transmission in a dental practice. The implications of signature polymorphisms seen within an infected individual, and shared polymorphisms between linked individuals, are also considered. VESPA may also be applied to the molecular analysis of biological phenotypes.

Published

1992

9. HIV-1 Sequence Variation Between Isolates from Mother-Infant Transmission Pairs

Author

Cecelia Hutto, Jose Munoz, Jean Baptiste Kurawige, Steven M. Wolinsky, Manohar Furtado, Carla M. Wike, Alfred J. Saah, Wade P. Parks, Michael R. Daniels, Marc Bulterys, and Bette T. Korber

Subjects

Adult, Genetics, Molecular Sequence Data, Immunology, Infant, Newborn, Genetic Variation, Mothers, HIV Infections, V3 loop, Biology, DNA sequencing, Virus, law.invention, Infectious Diseases, Transmission (mechanics), law, Virology, Genotype, HIV-1, Humans, Amino Acid Sequence, Genetic variability, Gene, Sequence (medicine)

Abstract

To examine the sequence diversity of human immunodeficiency virus type 1 (HIV-1) between known transmission sets, sequences from the V3 and V4-V5 region of the envelope gene from four mother-infant pairs were analyzed. The mean interpatient sequence variation between isolates from linked mother-infant pairs was comparable to the sequence diversity found between isolates from other close contacts. The mean intrapatient variation was significantly less in the infants' isolates then the isolates from both their mothers and other characterized intrapatient sequence sets. In addition, a distinct and characteristic difference in the glycosylation pattern preceding the V3 loop was found between each linked transmission pair. These findings indicate that selection of specific genotypic variants, which may play a role in some direct transmission sets, and the duration of infection are important factors in the degree of diversity seen between the sequence sets.

Published

1992

10. Targeting of a CD8 T cell env epitope presented by HLA-B*5802 is associated with markers of HIV disease progression and lack of selection pressure

Author

Dhanwanthie Ramduth, Daniel G. Kavanagh, Isobella Honeyborne, Hayley Crawford, Zenele Mncube, M van der Stok, David C. Nickle, Karen S. Bishop, Christine Rousseau, Eshia Moodley, Hoosen M. Coovadia, Nompumelelo Mkhwanazi, Nasreen Ismail, Kriebashnie Nair, Sharon Reddy, James I. Mullins, Philip J. R. Goulder, Bruce D. Walker, Christina F. Thobakgale, Kholiswa C. Ngumbela, C. de Pierres, Bette T. Korber, Cheryl L. Day, David Heckerman, and Photini Kiepiela

Subjects

T cell, Immunology, Molecular Sequence Data, Epitopes, T-Lymphocyte, Viremia, HIV Infections, Human leukocyte antigen, Biology, CD8-Positive T-Lymphocytes, Epitope, Virology, medicine, Cytotoxic T cell, Humans, Amino Acid Sequence, Antigen Presentation, Gene Products, env, Viral Load, medicine.disease, Infectious Diseases, medicine.anatomical_structure, HLA-B Antigens, Chronic Disease, Disease Progression, HIV-1, Viral disease, Viral load, CD8, Epitope Mapping

Abstract

In HIV-infected persons, certain HLA class I alleles are associated with effective control of viremia, while others are associated with rapid disease progression. Among the most divergent clinical outcomes are the relatively good prognosis in HLA-B*5801 expressing persons and poor prognosis with HLA-B*5802. These two alleles differ by only three amino acids in regions involved in HLA-peptide recognition. This study evaluated a cohort of over 1000 persons with chronic HIV clade C virus infection to determine whether clinical outcome differences associated with B*5801 (n = 93) and B*5802 ( n = 259) expression are associated with differences in HIV-1-specific CD8 (+) T cell responses. The overall breadth and magnitude of HIV-1-specific CD8(+) T cell responses were lower in persons expressing B*5802, and epitope presentation by B*5802 contributed significantly less to the overall response as compared to B*5801-restricted CD8 (+) T cells. Moreover, viral load in B*5802-positive persons was higher and CD4 cell counts lower when this allele contributed to the overall CD8 (+) T cell response, which was detected exclusively through a single epitope in Env. In addition, persons heterozygous for B*5802 compared to persons homozygous for other HLA-B alleles had significantly higher viral loads. Viral sequencing revealed strong selection pressure mediated through B*5801-restricted responses but not through B*5802. These data indicate that minor differences in HLA sequence can have a major impact on epitope recognition, and that selective targeting of Env through HLA-B*5802 is at least ineffectual if not actively adverse in the containment of viremia. These results provide experimental evidence that not all epitope-specific responses contribute to immune containment, a better understanding of which is essential to shed light on mechanisms involved in HIV disease progression.

Published

2008

11. Mother-to-child transmission in the United States of subtypes D and A/G human immunodeficiency virus type 1

Author

Yongzhi Geng, Susan H. Eshleman, George M. Johnson, Paul Krogstad, Sharon Nachman, Paul Palumbo, Michael Wantman, Dorothy Lang, Andrew Wiznia, Bette T. Korber, and J. Brooks Jackson

Subjects

Adolescent, Immunology, Population, Virus, Acquired immunodeficiency syndrome (AIDS), Pregnancy, Virology, medicine, Humans, Prospective Studies, education, Sida, Child, Phylogeny, education.field_of_study, Acquired Immunodeficiency Syndrome, biology, Transmission (medicine), business.industry, Infant, Viral Load, medicine.disease, biology.organism_classification, Infectious Disease Transmission, Vertical, Infectious Diseases, Child, Preschool, Lentivirus, HIV-1, Female, Viral disease, business, Viral load

Abstract

In the United States and Western Europe, most human immunodeficiency virus type 1 (HIV-1) infections are caused by subtype B. We analyzed the nucleotide sequence of HIV-1 RNA in plasma samples from 141 children enrolled into PACTG 377, a comparative study of several antiretroviral therapy regimens. Phylogenetic analysis revealed that two children, both born in the United States, were infected with non-B subtypes that are most commonly found in Africa: one with subtype D and the other with circulating recombinant form CRF02, an A/G recombinant lineage. Viral load assays performed to monitor treatment response underestimated the levels of HIV-1 RNA in the child with the A/G recombinant. These cases demonstrate mother-to-child transmission of non-B subtypes of HIV-1 in the United States. Non-B subtypes should be considered in the management of HIV-1-infected pregnant women and children to optimize strategies to prevent and treat pediatric HIV-1 infection.

Published

2002

12. HIV type 1 molecular clones able to use the Bonzo/STRL-33 coreceptor for virus entry

Author

Bette T. Korber, Yi-jun Zhang, Tom Ketas, Linqi Zhang, and John P. Moore

Subjects

CD4-Positive T-Lymphocytes, viruses, Placenta, Recombinant Fusion Proteins, Immunology, Molecular Sequence Data, Clone (cell biology), HIV Infections, Virus Replication, Genes, env, Virus, Cell Line, Receptors, G-Protein-Coupled, Viral entry, Virology, Humans, Amino Acid Sequence, Cloning, Molecular, Receptors, Cytokine, Gene, Tropism, Receptors, CXCR6, Genetics, biology, Infant, Newborn, virus diseases, Gene Products, env, Transfection, biology.organism_classification, Phenotype, Infectious Disease Transmission, Vertical, Infectious Diseases, Lentivirus, HIV-1, Leukocytes, Mononuclear, Receptors, Virus, Female, Receptors, Chemokine

Abstract

We describe the cloning of env genes from the mother-infant HIV-1 isolate pair P6-v3 and M6-v3. These viruses are unusual in that they can use the coreceptor Bonzo/STRL33 as well as CCR5 and, in the case of M6, CXCR4, to enter transfected cell lines in vitro. The phenotype of the parental isolates is generally reflected by the properties of the cloned env genes, when these are used in an Env-complementation assay of virus entry. Chimeric viruses were also made that contain the env genes of P6-v3 and M6-v3 inserted into the background of the infectious molecular clone, HIV-1 NL4-3. Some of the chimeric viruses derived from HIV1 P6-v3 were able to use Bonzo for entry into transfected cell lines, albeit to a lesser extent than they could use CCR5. There are some indications that one of these chimeric viruses, P6-v3-22-1, can use a coreceptor other than CCR5, perhaps Bonzo, to enter mitogen-stimulated PBMC, although only weakly. However, formal proof that this virus can use Bonzo in primary cells has not been obtained. The P6-v3-22-1 chimeric virus was unable to infect CD4-negative, placental cell lines, in the presence or absence of soluble CD4. Env sequence analysis revealed several differences among viruses with different tropisms, most notably a four amino acid deletion in the central region of the V3 loop that distinguishes the R5 virus P6-v3-25-4 from the R5, Bonzo virus P6-v3-22-1.

Published

2001

13. Associations between amino acids in the evolution of HIV type 1 protease sequences under indinavir therapy

Author

Jon H. Condra, Bette T. Korber, and Andrew J. Leigh Brown

Subjects

Nonsynonymous substitution, Time Factors, Genotype, medicine.medical_treatment, Immunology, HIV Infections, Indinavir, Biology, HIV Protease, Virology, Genetic variation, medicine, Humans, Amino Acid Sequence, Peptide sequence, Phylogeny, chemistry.chemical_classification, Genetics, Protease, Genetic Variation, Drug Resistance, Microbial, HIV Protease Inhibitors, Amino acid, Infectious Diseases, Enzyme, chemistry, Mutation, HIV-1, medicine.drug

Abstract

Significant diversity exists in amino acid sequences encoding HIV-1 protease in individuals naive for protease inhibitors, which could influence the rate of evolution of resistance. High-level resistance to indinavir requires multiple substitutions among at least 11 amino acid sites, and no single substitution was observed in all of 29 resistant isolates obtained from patients on long-term indinavir monotherapy. We have analyzed the evolution of PR in these sequences. The divergence from the baseline amino acid sequence by week 24 was 4%, increasing more than 7% by week 60. The mean difference between sequences from different patients at baseline was 6% (3-9%), rising to 10% after 40 weeks (3-16%), although at all time points nonsynonymous substitutions were less frequent than synonymous nucleotide changes. Analysis of associations between variants at different amino acid sites using a mutual information statistic revealed four pairs of sites to be significantly associated. In three cases these associations included residue 82. Clusters of baseline and week 24 amino acid sequences identified by maximum parsimony did not correlate significantly with the IC95 to indinavir, although a weak correlation of baseline clusters with phenotype at the week 24 time point was suggested.

Published

1999

14. Evaluation of different V3 peptides in an enzyme immunoassay for specific HIV type 1 group O antibody detection

Author

François Simon, Katrien Fransen, Sentob Saragosti, John N. Nkengasong, B. Willems, Wouter Janssens, Lutz G. Gürtler, Leo Heyndrickx, Bette T. Korber, Pascale Ondoa, Jaap Goudsmit, G van der Groen, Leopold Zekeng, Martine Peeters, Peter M. Ndumbe, and Other departments

Subjects

Male, Immunology, Gene Products, pol, Peptide, HIV Infections, V3 loop, HIV Antibodies, HIV Envelope Protein gp120, Sensitivity and Specificity, Immunoenzyme Techniques, Viral envelope, Virology, Consensus sequence, medicine, Humans, Cameroon, chemistry.chemical_classification, biology, medicine.diagnostic_test, Molecular biology, Peptide Fragments, Amino acid, Europe, Infectious Diseases, Enzyme, chemistry, Evaluation Studies as Topic, Immunoassay, biology.protein, HIV-1, Female, Antibody, Peptides

Abstract

Strategies to discriminate group O from group M infections need to be improved. We have developed and evaluated an HIV-1 group O V3 peptide-based enzyme immunoassay (PEIA) for specific HIV-1 group O antibody detection among HIV-1-infected patients. Synthetic peptides, derived from the amino acid sequences of the V3 loop of 15 different group O strains and 7 group O consensus sequences, were evaluated in a PEIA against a panel of genetically confirmed group O (n = 33), group M (n = 90), and HIV-1 antibody-negative sera (n = 17). The best-performing PEIA(s) were then used to screen 134 sera of European and 336 sera of Cameroonian origin for the presence of anti-HIV-1 group O antibodies. The reactivity of reference ("gold standard") sera to individual peptides in the PEIA resulted in the selection of five different peptides with sensitivities (sens), specificities (spec), and test efficiencies (TEs) in the range of 90 to 100%. Improvement of the PEIA was obtained with simultaneous reactivity of at least two different peptides in separate wells of an ELISA plate, together with stringent criteria for positivity. We were able to select seven peptide combinations each with a sens, spec, and TE of 96.9, 100, and 99.2%, respectively. None of the 134 European and 4 (1.2%) of the 336 Cameroonian samples sera were group O positive in the optimized HIV-1 group O PEIA; this was confirmed by the repeated presence of reactives, in agreement with the present knowledge of group O infection distribution. Finally, we were able to develop a strategy with a higher TE (99.2%) than the previously used ANT-70 (98.5%) and ANT-70/MVP5180 (95.7%). Our results show that optimal specificity rather than optimal sensitivity makes the V3 PEIA a sufficiently accurate epidemiological tool to be useful in estimating specifically group O infection among HIV-1-infected patients.

Published

1998

15. A computer program designed to screen rapidly for HIV type 1 intersubtype recombinant sequences

Author

Aaron L. Halpern, Bette T. Korber, Adam Siepel, and Catherine A. Macken

Subjects

Recombination, Genetic, Base Sequence, Immunology, Molecular Sequence Data, Human immunodeficiency virus (HIV), Biology, medicine.disease_cause, Virology, Genes, env, Genes, gag, law.invention, Infectious Diseases, law, Computer software, DNA, Viral, Recombinant DNA, medicine, HIV-1, Humans, Phylogeny, Software

Abstract

n/a

Published

1995

16. Diversity of V3 region sequences of human immunodeficiency viruses type 1 from the central African Republic

Author

Marie-Claude Georges-Courbot, Debra Cook, Marc Girard, Bruno You, Françoise Barré-Sinoussi, Bette T. Korber, Ellen Murphy, Abraham Pinter, Alain J. Georges, Christian Mathiot, and Marie-Paule Kieny

Subjects

Male, Sequence analysis, Immunology, Molecular Sequence Data, Human immunodeficiency virus (HIV), Biology, HIV Envelope Protein gp120, medicine.disease_cause, Virus, Type (biology), Phylogenetics, Virology, Genetic variation, medicine, Humans, Amino Acid Sequence, Phylogeny, Acquired Immunodeficiency Syndrome, Base Sequence, Sequence Homology, Amino Acid, Central africa, Genetic Variation, Sequence Analysis, DNA, Central African Republic, Infectious Diseases, HIV-1, Female, Viral disease

Abstract

Nucleotide sequences of the central portion of gp120, including the third hypervariable (V3) loop, were obtained from lymphocytes cocultivated with SupT1 cells from 29 AIDS patients in Bangui, Central African Republic. These sequences displayed significantly greater diversity (average distance, 23%) than has been previously observed in isolates from comparably restricted geographical areas. Isolates belonging to four major subtypes of HIV-1 were found; the only subtype not represented was the North American/European subtype B. Unlike the situation in Zaire and Uganda, where subtypes A and D account equally for virtually all isolates of HIV-1, the predominant subtypes in the Central African Republic, accounting for two-thirds of the isolates, were subtypes A (10 isolates) and E (9 isolates). Subtype E represents a group of variants that have previously been found only in Thailand. Only one isolate belonging to subtype D was found. Also recovered were two isolates of subtype C, a subtype associated with southern African and Indian isolates but not previously detected in central Africa. These isolates, although clearly clustering with subtype C, formed a distinct subset, differing from one another by 8.8% and from the Indian and South African subtype C isolates by an average of 22.5%. High interpatient, intrasubtype variation was also seen among the CAR subtype A (average pairwise difference, 19.3%) and subtype E (10.9%) isolates. The diversity of V3 sequences in this set has implications for immunization protocols that rely on the recognition of V3. This study underscores the necessity of basing intervention strategies on knowledge of the particular sequences present in the target population or geographical area.

Published

1993

17. The emergence of simian/human immunodeficiency viruses

Author

Gerald Myers, Kersti MacINNES, and Bette T. Korber

Subjects

Genes, Viral, viruses, Immunology, Biology, Simian, medicine.disease_cause, Virus, chemistry.chemical_compound, Viral Proteins, Viral Envelope Proteins, Phylogenetics, Virology, medicine, Gene, Immunodeficiency, Phylogeny, Genetics, Phylogenetic tree, HIV, Simian immunodeficiency virus, medicine.disease, biology.organism_classification, Infectious Diseases, chemistry, DNA, Viral, Simian Immunodeficiency Virus, DNA

Abstract

Molecular evolutionary analyses strongly support the hypothesis that human immunodeficiency viruses have recently arisen from a diverse pool of nonhuman primate immunodeficiency viruses. Our understanding of the molecular phylogenetic relationships between primate and nonprimate lentiviruses is less certain, partly because key intermediate forms are still to be discovered. DNA and protein sequence comparisons reveal uncanny dissimilarities, as well as similarities, among the genetic sequences of these complex retroviruses, thereby giving rise to the notion that primate lentiviruses are participants in "fast-forward" evolution.

Published

1992

18. Comment to the Letter to the Editor

Author

Christian Brander, Bruce D. Walker, and Bette T. Korber

Subjects

Infectious Diseases, Letter to the editor, Virology, Philosophy, Immunology, Classics

Published

1998