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抗逆转录病毒耐药性的国际视角。非核苷类逆转录酶抑制剂耐药性。

International perspectives on antiretroviral resistance. Nonnucleoside reverse transcriptase inhibitor resistance.

作者信息

Deeks S G

机构信息

San Francisco General Hospital, San Francisco, California and University of California, San Francisco, California, USA.

出版信息

J Acquir Immune Defic Syndr. 2001 Mar 1;26 Suppl 1:S25-33. doi: 10.1097/00042560-200103011-00004.

Abstract

Although understanding of nonnucleoside reverse transcriptase inhibitor (NNRTI) resistance is less clearly established than that of other classes of antiretroviral drugs, certain facts have been established. The treatment-associated genetic mutation profiles of the available NNRTIs have been mapped, and resistance has been found to develop rapidly after initiation of NNRTI therapy. Despite the chemical diversity of the NNRTIs, cross-resistance among agents of this class is nearly universal. Although the viral replicative capacity ("fitness") of NNRTI-induced viral variants has not been extensively studied, available data suggest that NNRTI-selected mutations confer little damage to viral fitness, and thus a single point mutation produces a strain that is both resistant and fit. Furthermore, with continued therapy, viral evolution persists, creating species with greater numbers of mutations and higher level phenotypic resistance. Taken together, these facts suggest that continued use of NNRTIs after emergence of resistance will produce variants of complex mutational patterns that limit future treatment options, and, therefore, strong consideration should be given to discontinuing NNRTIs after virologic failure is confirmed. This article describes the scientific literature establishing the efficacy and limitations of NNRTI therapy and attempts to define a role for this class of drug in the long-term treatment of HIV-1 disease.

摘要

尽管对非核苷类逆转录酶抑制剂(NNRTI)耐药性的了解不如对其他类抗逆转录病毒药物那样明确,但一些事实已经明确。已绘制出可用的NNRTIs与治疗相关的基因突变图谱,并且发现耐药性在开始NNRTI治疗后迅速出现。尽管NNRTIs在化学结构上具有多样性,但该类药物之间的交叉耐药几乎是普遍存在的。虽然对NNRTI诱导的病毒变体的病毒复制能力(“适应性”)尚未进行广泛研究,但现有数据表明,NNRTI选择的突变对病毒适应性造成的损害很小,因此单个点突变就会产生既耐药又具有适应性的毒株。此外,随着治疗的持续,病毒进化持续存在,产生具有更多突变和更高水平表型耐药性的毒株。综上所述,这些事实表明,耐药性出现后继续使用NNRTIs将产生具有复杂突变模式的变体,从而限制未来的治疗选择,因此,在确认病毒学失败后,应强烈考虑停用NNRTIs。本文描述了确立NNRTI治疗的疗效和局限性的科学文献,并试图界定这类药物在HIV-1疾病长期治疗中的作用。

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