Your search keyword '"Tania Escamilla-Gomez"' showing total 2 results

1. Novel HLA class I associations with HIV-1 control in a unique genetically admixed population

Author

Santiago Ávila-Ríos, Carlos Quant-Durán, Mark A. Brockman, Ingrid Y. Escobar-Urias, Zabrina L. Brumme, Francisco-Javier Prado-Galbarro, Ramón Hernández-Juan, Guillermo Porras-Cortés, Tania Escamilla-Gomez, Thalia Garcia-Tellez, Carmen Aláez, Edna Rodríguez-Aguirre, Gustavo Reyes-Terán, Daniela Garrido-Rodríguez, Akio Murakami-Ogasawara, Rolando A Cedillos, Silvia J Del Arenal-Sánchez, Humberto Valenzuela-Ponce, Daniela Tapia-Trejo, Claudia García-Morales, P. Richard Harrigan, Chanson J. Brumme, Elsa Palou, Maribel Soto-Nava, Rita I Meza, Selma Alva-Hernández, Juan Miguel Pascale, Yamitzel Zaldivar, Verónica S Quiroz-Morales, Ivette Lorenzana, Rodolfo Pinzón-Meza, Marvin Manzanero, and Carlos Mejía-Villatoro

Subjects

Adult, Male, 0301 basic medicine, Canada, Linkage disequilibrium, Genotype, Population, lcsh:Medicine, Genetic admixture, HIV Infections, Human leukocyte antigen, Biology, Article, Linkage Disequilibrium, Cohort Studies, Young Adult, 03 medical and health sciences, Gene Frequency, HLA Antigens, Polymorphism (computer science), Humans, Allele, lcsh:Science, education, Mexico, Allele frequency, Genetics, education.field_of_study, Polymorphism, Genetic, Multidisciplinary, lcsh:R, Central America, 3. Good health, Genetics, Population, 030104 developmental biology, HIV-1, Female, lcsh:Q

Abstract

Associations between HLA class I alleles and HIV progression in populations exhibiting Amerindian and Caucasian genetic admixture remain understudied. Using univariable and multivariable analyses we evaluated HLA associations with five HIV clinical parameters in 3,213 HIV clade B-infected, ART-naïve individuals from Mexico and Central America (MEX/CAM cohort). A Canadian cohort (HOMER, n = 1622) was used for comparison. As expected, HLA allele frequencies in MEX/CAM and HOMER differed markedly. In MEX/CAM, 13 HLA-A, 24 HLA-B, and 14 HLA-C alleles were significantly associated with at least one clinical parameter. These included previously described protective (e.g. B*27:05, B*57:01/02/03 and B*58:01) and risk (e.g. B*35:02) alleles, as well as novel ones (e.g. A*03:01, B*15:39 and B*39:02 identified as protective, and A*68:03/05, B*15:30, B*35:12/14, B*39:01/06, B*39:05~C*07:02, and B*40:01~C*03:04 identified as risk). Interestingly, both protective (e.g. B*39:02) and risk (e.g. B*39:01/05/06) subtypes were identified within the common and genetically diverse HLA-B*39 allele group, characteristic to Amerindian populations. While HLA-HIV associations identified in MEX and CAM separately were similar overall (Spearman’s rho = 0.33, p = 0.03), region-specific associations were also noted. The identification of both canonical and novel HLA/HIV associations provides a first step towards improved understanding of HIV immune control among unique and understudied Mestizo populations.

Published

2018

2. In vitro functional assessment of natural HIV-1 group M Vpu sequences using a universal priming approach

Author

Zabrina L. Brumme, Tristan J. Markle, Gursev Anmole, David R. Bangsberg, Guinevere Q. Lee, Gustavo Reyes-Terán, Santiago Ávila-Ríos, Steven W. Jin, P. Richard Harrigan, Maribel Soto-Nava, Mark A. Brockman, Asa Rahimi, Jeffrey N. Martin, and Tania Escamilla-Gomez

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, animal diseases, viruses, Response element, Human Immunodeficiency Virus Proteins, Down-Regulation, Sequence diversity, HIV Infections, Biology, Response Elements, Microbiology, Article, 03 medical and health sciences, Clinical Research, Virology, Genetic variation, Genotype, Genetics, Coding region, Humans, Viral Regulatory and Accessory Proteins, DNA Primers, Genetic diversity, BST2/tetherin, HIV-1 Vpu, virus diseases, Genetic Variation, Nucleic acid amplification technique, biochemical phenomena, metabolism, and nutrition, Phenotype, In vitro, CD4, Rev/RRE, 030104 developmental biology, Medical Microbiology, Downregulation, HIV-1, HIV/AIDS, Infection, Nucleic Acid Amplification Techniques, Biotechnology

Abstract

The HIV-1 accessory protein Vpu exhibits high inter- and intra- subtype genetic diversity that may influence Vpu function and possibly contribute to HIV-1 pathogenesis. However, scalable methods to evaluate genotype/phenotype relationships in natural Vpu sequences are limited, particularly those expressing the protein in CD4+ T-cells, the natural target of HIV-1 infection. A major impediment to assay scalability is the extensive genetic diversity within, and immediately upstream of, Vpu's initial 5' coding region, which has necessitated the design of oligonucleotide primers specific for each individual HIV-1 isolate (or subtype). To address this, we developed two universal forward primers, located in relatively conserved regions 38 and 90 bases upstream of Vpu, and a single universal reverse primer downstream of Vpu, which are predicted to cover the vast majority of global HIV-1 group M sequence diversity. We show that inclusion of up to 90 upstream bases of HIV-1 genomic sequence does not significantly influence in vitro Vpu expression or function when a Rev/Rev Response Element (RRE)-dependent expression system is used. We further assess the function of four diverse HIV-1 Vpu sequences, revealing reproducible and significant differences between them. Our approach represents a scalable option to measure the in vitro function of genetically diverse natural Vpu isolates in a CD4+ T-cell line.

Published

2017