Sylvia Stack scite author profile

Sylvia Stack

3Publications

66Citation Statements Received

0Citation Statements Given

How they've been cited

109

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Affiliations

DuPont (United States), Experimental Station, MSD (United States)

Publications

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Limited Sequence Diversity of the HIV Type 1 Protease Gene from Clinical Isolates andin VitroSusceptibility to HIV Protease Inhibitors

Winslow

Stack²,

King³

et al. 1995

AIDS Research and Human Retroviruses

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Proviral DNAs from 3 laboratory strains and 21 clinical isolates of HIV-1 were extracted from infected cells after proteinase K digestion and the protease gene was PCR amplified and sequenced directly by the Sanger method. In vitro susceptibilities of the virus isolates to protease inhibitors were determined by the ACTG/DoD consensus assay. Four different HIV protease inhibitors were tested including P9941, a C2 symmetrical diol (Du Pont-Merck); A80987, an asymmetric mono-ol (Abbott); XM323, a cyclic urea (Du Pont-Merck); and Ro31-8959, an asymmetric hydroxyethylene isostere (Roche). Maximum sequence variation was 10% at both the nucleic and amino acid levels. Purine-purine substitutions were most common. Five noncontiguous regions were conserved across all isolates and corresponded to amino acids 1-9 (amino terminal), 21-32 (catalytic site), 47-56 ("flap" region), 78-88 (substrate-binding region), and 94-99 (carboxy terminal). All clinical isolates demonstrated in vitro susceptibility to the protease inhibitors. There was no significant difference between the susceptibility of the reference strains and the clinical isolates. These data suggest that the variable regions of protease do not contain sites that are important for interactions with the inhibitors tested.

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Cloning, expression and tissue distribution of the gene encoding rat fibroblast growth factor receptor subtype 4

Horlick

Stack

Cooke

1992

Gene

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Identification of a clinical isolate of HIV-1 with an isoleucine at position 82 of the protease which retains susceptibility to protease inhibitors

et al. 1995

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Sylvia Stack

Limited Sequence Diversity of the HIV Type 1 Protease Gene from Clinical Isolates andin VitroSusceptibility to HIV Protease Inhibitors

Cloning, expression and tissue distribution of the gene encoding rat fibroblast growth factor receptor subtype 4

Identification of a clinical isolate of HIV-1 with an isoleucine at position 82 of the protease which retains susceptibility to protease inhibitors

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