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抗病毒活性与宿主毒性之间的关系:1型人类免疫缺陷病毒逆转录酶和人类线粒体DNA聚合酶对2',3'-二脱氧-5-氟-3'-硫代胞苷三磷酸类似物掺入效率的比较

Relationship between antiviral activity and host toxicity: comparison of the incorporation efficiencies of 2',3'-dideoxy-5-fluoro-3'-thiacytidine-triphosphate analogs by human immunodeficiency virus type 1 reverse transcriptase and human mitochondrial DNA polymerase.

作者信息

Feng Joy Y, Murakami Eisuke, Zorca Suzana M, Johnson Allison A, Johnson Kenneth A, Schinazi Raymond F, Furman Phillip A, Anderson Karen S

机构信息

Gilead Sciences, Durham, North Carolina 27707, USA.

出版信息

Antimicrob Agents Chemother. 2004 Apr;48(4):1300-6. doi: 10.1128/AAC.48.4.1300-1306.2004.

Abstract

Emtricitabine [(-)FTC; (-)-beta-L-2'-3'-dideoxy-5-fluoro-3'-thiacytidine] is an oxathiolane nucleoside analog recently approved by the Food and Drug Administration for the treatment of human immunodeficiency virus (HIV). Structurally, (-)FTC closely resembles lamivudine [(-)3TC] except that the former is 5-fluorinated on the cytosine ring. In HIV-1 reverse transcriptase (RT) enzymatic assays, the triphosphate of (-)FTC [(-)FTC-TP] was incorporated into both DNA-DNA and DNA-RNA primer-templates nearly 3- and 10-fold more efficiently than (-)3TC-TP. Animal studies and clinical trial studies have demonstrated a favorable safety profile for (-)FTC. However, a detailed study of the incorporation of (-)FTC-TP by human mitochondrial DNA polymerase gamma, a host enzyme associated with nucleoside toxicity, is required for complete understanding of the molecular mechanisms of inhibition and toxicity. We studied the incorporation of (-)FTC-TP and its enantiomer (+)FTC-TP into a DNA-DNA primer-template by recombinant human mitochondrial DNA polymerase in a pre-steady-state kinetic analysis. (-)FTC-TP was incorporated 2.9 x 10(5)-, 1.1 x 10(5)-, 1.6 x 10(3)-, 7.9 x 10(3)-, and 100-fold less efficiently than dCTP, ddCTP, (+)3TC-TP, (+)FTC-TP, and (-)3TC-TP, respectively. The rate of removal of (-)FTC-MP from the corresponding chain-terminated 24-mer DNA by polymerase gamma's 3'-->5' exonuclease activity was equal to the removal of (+)FTC-MP, 2-fold slower than the removal of (-)3TC-MP and (+)3TC-MP, and 4.6-fold slower than the excision of dCMP. These results demonstrate that there are clear differences between HIV-1 RT and polymerase gamma in terms of preferences for substrate structure.

摘要

恩曲他滨[(-)FTC;(-)-β-L-2'-3'-二脱氧-5-氟-3'-硫代胞苷]是一种氧硫杂环戊烷核苷类似物,最近被美国食品药品监督管理局批准用于治疗人类免疫缺陷病毒(HIV)。在结构上,(-)FTC与拉米夫定[(-)3TC]非常相似,只是前者在胞嘧啶环上有5-氟取代。在HIV-1逆转录酶(RT)酶促试验中,(-)FTC的三磷酸酯[(-)FTC-TP]掺入DNA-DNA和DNA-RNA引物模板的效率分别比(-)3TC-TP高近3倍和10倍。动物研究和临床试验研究表明(-)FTC具有良好的安全性。然而,为了全面了解抑制和毒性的分子机制,需要对人线粒体DNA聚合酶γ(一种与核苷毒性相关的宿主酶)掺入(-)FTC-TP进行详细研究。我们在预稳态动力学分析中,通过重组人线粒体DNA聚合酶研究了(-)FTC-TP及其对映体(+)FTC-TP掺入DNA-DNA引物模板的情况。(-)FTC-TP掺入的效率分别比dCTP、ddCTP、(+)3TC-TP、(+)FTC-TP和(-)3TC-TP低2.9×10⁵倍、1.1×10⁵倍、1.6×10³倍、7.9×10³倍和100倍。聚合酶γ的3'→5'核酸外切酶活性从相应的链终止24聚体DNA中去除(-)FTC-MP的速率与去除(+)FTC-MP的速率相等,比去除(-)3TC-MP和(+)3TC-MP的速率慢2倍,比切除dCMP的速率慢4.6倍。这些结果表明,HIV-1 RT和聚合酶γ在底物结构偏好方面存在明显差异。

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