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Natural variation of HIV-1 group M integrase: implications for a new class of antiretroviral inhibitors.


ABSTRACT: HIV-1 integrase is the third enzymatic target of antiretroviral (ARV) therapy. However, few data have been published on the distribution of naturally occurring amino acid variation in this enzyme. We therefore characterized the distribution of integrase variants among more than 1,800 published group M HIV-1 isolates from more than 1,500 integrase inhibitor (INI)-naïve individuals. Polymorphism rates equal or above 0.5% were found for 34% of the central core domain positions, 42% of the C-terminal domain positions, and 50% of the N-terminal domain positions. Among 727 ARV-naïve individuals in whom the complete pol gene was sequenced, integrase displayed significantly decreased inter- and intra-subtype diversity and a lower Shannon's entropy than protease or RT. All primary INI-resistance mutations with the exception of E157Q--which was present in 1.1% of sequences--were nonpolymorphic. Several accessory INI-resistance mutations including L74M, T97A, V151I, G163R, and S230N were also polymorphic with polymorphism rates ranging between 0.5% to 2.0%.

SUBMITTER: Rhee SY 

PROVIDER: S-EPMC2546438 | biostudies-literature | 2008 Aug

REPOSITORIES: biostudies-literature

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Natural variation of HIV-1 group M integrase: implications for a new class of antiretroviral inhibitors.

Rhee Soo-Yon SY   Liu Tommy F TF   Kiuchi Mark M   Zioni Rafael R   Gifford Robert J RJ   Holmes Susan P SP   Shafer Robert W RW  

Retrovirology 20080807


HIV-1 integrase is the third enzymatic target of antiretroviral (ARV) therapy. However, few data have been published on the distribution of naturally occurring amino acid variation in this enzyme. We therefore characterized the distribution of integrase variants among more than 1,800 published group M HIV-1 isolates from more than 1,500 integrase inhibitor (INI)-naïve individuals. Polymorphism rates equal or above 0.5% were found for 34% of the central core domain positions, 42% of the C-termina  ...[more]

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