Your search keyword '"Anh Q. Le"' showing total 2 results

1. Ability of HIV-1 Nef to downregulate CD4 and HLA class I differs among viral subtypes.

Author

Mann, Jaclyn K., Byakwaga, Helen, Xiaomei T. Kuang, Anh Q. Le, Brumme, Chanson J., Mwimanzi, Philip, Omarjee, Saleha, Martin, Eric, Lee, Guinevere Q., Baraki, Bemuluyigza, Danroth, Ryan, McCloskey, Rosemary, Muzoora, Conrad, Bangsberg, David R., Hunt, Peter W., Goulder, Philip J. R., Walker, Bruce D., Richard Harrigan, P., Martin, Jeff N., and Thumbi Ndung'u

Subjects

NEF gene, PAPILLOMAVIRUS pathogenicity, HIV infections, GENETIC code, HLA histocompatibility antigens

Abstract

Background: The highly genetically diverse HIV-1 group M subtypes may differ in their biological properties. Nef is an important mediator of viral pathogenicity; however, to date, a comprehensive inter-subtype comparison of Nef in vitro function has not been undertaken. Here, we investigate two of Nef's most well-characterized activities, CD4 and HLA class I downregulation, for clones obtained from 360 chronic patients infected with HIV-1 subtypes A, B, C or D. Results: Single HIV-1 plasma RNA Nef clones were obtained from N=360 antiretroviral-naïve, chronically infected patients from Africa and North America: 96 (subtype A), 93 (B), 85 (C), and 86 (D). Nef clones were expressed by transfection in an immortalized CD4+ T-cell line. CD4 and HLA class I surface levels were assessed by flow cytometry. Nef expression was verified by Western blot. Subset analyses and multivariable linear regression were used to adjust for differences in age, sex and clinical parameters between cohorts. Consensus HIV-1 subtype B and C Nef sequences were synthesized and functionally assessed. Exploratory sequence analyses were performed to identify potential genotypic correlates of Nef function. Subtype B Nef clones displayed marginally greater CD4 downregulation activity (p = 0.03) and markedly greater HLA class I downregulation activity (p < 0.0001) than clones from other subtypes. Subtype C Nefs displayed the lowest in vitro functionality. Inter-subtype differences in HLA class I downregulation remained statistically significant after controlling for differences in age, sex, and clinical parameters (p < 0.0001). The synthesized consensus subtype B Nef showed higher activities compared to consensus C Nef, which was most pronounced in cells expressing lower protein levels. Nef clones exhibited substantial inter-subtype diversity: cohort consensus residues differed at 25% of codons, while a similar proportion of codons exhibited substantial inter-subtype differences in major variant frequency. These amino acids, along with others identified in intra-subtype analyses, represent candidates for mediating inter-subtype differences in Nef function. Conclusions: Results support a functional hierarchy of subtype B > A/D > C for Nef-mediated CD4 and HLA class I downregulation. The mechanisms underlying these differences and their relevance to HIV-1 pathogenicity merit further investigation. [ABSTRACT FROM AUTHOR]

Published

2013

2. Limited evidence for alterations in Gag-mediated HIV replication capacity over the course of the North American epidemic (1979-present)

Author

Simon Mallal, Zabrina L. Brumme, Mark A. Brockman, Susan Buchbinder, Kenneth H. Mayer, Mina John, Jonathan D. Fuchs, Bruce D. Walker, Art F. Y. Poon, T. Kuang, Theresa Wagner, Anh Q. Le, Eric Martin, Laura A. Cotton, Beryl A. Koblin, Kali A. Penney, Jonathan M. Carlson, and Denis Chopera

Subjects

Genetics, lcsh:Immunologic diseases. Allergy, Mutation, education.field_of_study, Population, Human leukocyte antigen, Biology, medicine.disease_cause, Virology, law.invention, Immune system, Infectious Diseases, law, Poster Presentation, Cohort, medicine, Recombinant DNA, biology.protein, Antibody, education, lcsh:RC581-607, Allele frequency

Abstract

Background: The extent to which HIV replication capacity (RC) has changed over the epidemic’s course, and the influence of HLA-associated immune pressure as its driving force remains unknown. We performed a comparative study of immune escape and RC in historic (1979-1989) and modern Gag subtype B sequences from North America. Methods: Using phylogenetically-informed methods, we identified HLA-associated Gag polymorphisms in a historic cohort (N=239; 1979-1989). We also generated recombinant NL4-3 viruses encoding clonal plasma RNA Gag from 80 historic and 58 modern (2002-2008) sequences. Viral RC was measured using a GFP reporter T-cell assay and results were normalized to NL4-3 controls. Results: 95% of HLA-associated polymorphisms identified in the historic cohort were consistent with published modern escape pathways. Overall, the prevalence of HLA-associated polymorphisms in the general population increased a median 1.3-fold between historic and modern sequences; however in many cases this was influenced by differences in HLA allele frequencies between HIV-infected populations examined. Of note, the prevalence of the B*27-associated R264K escape mutation increased from 0.4 to 1.3% in the general population over time despite B*27 allele frequency remaining constant at 2.5%. Modestly lower viral RC was observed for Gag recombinant viruses constructed from pre-1985 sequences (median 0.86 [IQR 0.78-0.97], N=24) compared to those from 1985-1989 (median 0.98 [IQR 0.87-1.05], N=56) and 2002-2008 (median 0.96 [IQR 0.83-0.1.10], N=58) (p=0.049). In both historic and modern cohorts, host expression of HLA-B*27 was associated with lower RC (p=0.007). Gag codons associated with lower RC, including S67A, were identified in an exploratory analysis. Conclusion: Gag-mediated viral RC may have increased modestly since the beginning of the North American epidemic, despite limited evidence for HLA-driven viral sequence evolution during this time. Although mechanisms driving RC differences remain unclear, results do not support rapid and substantial accumulation of HLA-driven escape mutations in circulating North American HIV-1 sequences.