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. 2020 Feb;36(2):161-166.
doi: 10.1089/AID.2019.0201. Epub 2019 Oct 24.

Mexican HIV-1 Protease Sequence Diversity

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Mexican HIV-1 Protease Sequence Diversity

Pedro G Hernandez-Sanchez et al. AIDS Res Hum Retroviruses. 2020 Feb.

Abstract

Protease is one of three enzymes encoded within HIV's pol gene, responsible for the cleavage of viral Gag-Pol polypeptide into mature viral proteins and a target of current anti-retroviral therapy. Protease diversity analysis in Latin America has been lacking in spite of extensive studies of protease-inhibitor resistance mutations. We studied the diversity of 777 Mexican protease sequences and found that all were subtype B except one (CRF02_AG). Phylogenetic analysis suggested the existence of six different clades with geospecific contributions. Thirty-three percent of sites were conserved, 25% had conservative substitutions, and 41% exhibited physicochemical changes. The most conserved regions surrounded the active site, most of the flap domain, and a region between the 60's loop and C-terminal triad. A single sequence exhibited an active site mutation (T26S). Variable sites were mapped to a crystallographic structure, providing further insight into the distribution and functional relevance of variable sites among Mexican isolates.

Keywords: Mexico; anti-retroviral mutations; genetic diversity; molecular modelling; protease.

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