literature

HIV mutation literature information.

Polymorphisms of HIV-2 integrase and selection of resistance to raltegravir.

PMID: 21114823 2010 Retrovirology

Introduction: RAL resistance is not well documented for HIV-2, although cases of therapy failure have been associated with the emergence of variants carrying the Y143C, Q148K/R, or N155 H mutations, including Y143Y+T97A or Q148K, or Q148R+G140 S.

Extended use of raltegravir in the treatment of HIV-1 infection: optimizing therapy.

PMID: 21694899 2010 Infection and drug resistance

Discussion: The secondary mutations G140A/S, E92Q, and T97A are preferentially linked to the Q148, N155, and Y143 genetic pathways, respectively.

HIV-1 integrase polymorphisms are associated with prior antiretroviral drug exposure.

PMID: 19203393 2009 Retrovirology

Introduction: T97A, V151I, G163R, I203M and S230N) remains unknown.

Introduction: However, in a small study conducted at Westmead Hospital, Sydney, Australia, G140S was detected in 2 INI-naive patients, as were the other accessory mutations: L74I/M (n = 8), T97A (n = 2), V151I (n = 3) and I203M (n = 4).

Characterization and structural analysis of HIV-1 integrase conservation.

PMID: 19290031 2009 AIDS reviews

Abstract: Differently, other mutations (L74M, T97A, S119G/R, V151I, K156N, E157Q, G163K/R, V165I, I203M, T206S, S230N) occurred as natural polymorphisms with a different prevalence according to different HIV-1 subtype/circulating recombinant form/group.

Analysis of pol integrase sequences in diverse HIV type 1 strains using a prototype genotyping assay.

PMID: 19327053 2009 AIDS research and human retroviruses

Abstract: Some samples had other mutations selected by these drugs including T97A, and some had amino acid polymorphisms at positions associated with raltegravir and elvitegravir resistance.

Evolution of raltegravir resistance during therapy.

PMID: 19447792 2009 The Journal of antimicrobial chemotherapy

Abstract: The secondary mutations L74M, T97A, V151I and G163R were observed with a frequency of <4%.

Natural polymorphisms of human immunodeficiency virus type 1 integrase and inherent susceptibilities to a panel of integrase inhibitors.

PMID: 19651917 2009 Antimicrobial agents and chemotherapy

Abstract: We identified polymorphisms V72I, L74I, T97A, V151I, M154I/L, E157Q, V165I, V201I, I203M, T206S, and S230N.

Effects of HIV type-1 immune selection on susceptability to integrase inhibitor resistance.

PMID: 19918099 2009 Antiviral therapy

Result: These seven sites were L74I/M at the C terminus of HLA-B*1510-restricted THLEGKIIL, 91 at p9 of YIEAEVIPA with unknown restriction, T97A at p2 of HLA-A*2601-restricted ETGQETAY, 126 at p9 of HLA-A*3002-restricted KIQNFRYY, 128 at p2 of HLA-A2-restricted AKAACWWAGI, 143 at p9 of HLA-B*1503-restricted KQEFGIPY and 165 at p2 of HLA-A*0205-restricted QVRDQAEHL.

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

PMID: 18687142 2008 Retrovirology

Abstract: 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%.

Result: Among mutations selected by raltegravir or elvitegravir that have not been shown to directly reduce susceptibility, L74R, Q95K, E138A/K, and H183P were conserved, whereas V54I, L68V, L74M, T97A, V151I, G163R, and I203M

Natural polymorphism of the HIV-1 integrase gene and mutations associated with integrase inhibitor resistance.

PMID: 17668566 2007 Antiviral therapy

Abstract: Of the 42 aa substitutions currently associated with INI resistance, 21 occurred as natural polymorphisms: V72I, L74I, T97A, T112I, A128T, E138K, Q148H, V151I, S153Y/A, M154I, N155H, K156N, E157Q, G163R, V165I, V201I, I203M, T206S, S230N and R263K.

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