逆转录酶突变118I、208Y和215Y导致HIV-1对非核苷类逆转录酶抑制剂高度敏感。

Reverse transcriptase mutations 118I, 208Y, and 215Y cause HIV-1 hypersusceptibility to non-nucleoside reverse transcriptase inhibitors.

作者信息

Clark Shauna A, Shulman Nancy S, Bosch Ronald J, Mellors John W

机构信息

School of Medicine, University of Pittsburgh, 3550 Terrace Street, Pittsburgh, PA 15261, USA.

出版信息

AIDS. 2006 Apr 24;20(7):981-4. doi: 10.1097/01.aids.0000222069.14878.44.

DOI:10.1097/01.aids.0000222069.14878.44

PMID:16603849

Abstract

BACKGROUND

HIV-1 hypersusceptibility to non-nucleoside reverse transcriptase inhibitors (NNRTI) improves the response to NNRTI-containing regimens. The genetic basis for NNRTI hypersusceptibility was partly defined in our earlier analyses of a paired genotype-phenotype dataset of viral isolates from treatment-experienced patients, in which we identified reverse transcriptase mutations V118I, H208Y, and T215Y as being strongly associated with NNRTI hypersusceptibility.

OBJECTIVES

We evaluated the role of these mutations in NNRTI hypersusceptibility by site-directed mutagenesis and phenotypic analysis of HIV-1 recombinants.

METHODS

Drug susceptibility and replication capacity were determined in single cycle assays. Hypersusceptibility was defined by a statistically significant (P < 0.01; Student's t-test) mean fold-change in 50% inhibitory concentration (IC50) of less than 0.4.

RESULTS

The single mutations V118I, H208Y, and T215Y did not show hypersusceptibility to efavirenz with mean fold-change of 0.58, 0.55, and 0.70, respectively (P < 0.01 and P = 0.12). The H208Y/T215Y and V118I/H208Y/T215Y mutants showed marked hypersusceptibility to efavirenz, having mean fold-change values of 0.27 and 0.20, respectively (P < 0.001). In addition, H208Y/T215Y, V118I/T215Y, and V118I/H208Y/T215Y were hypersusceptible to delavirdine and nevirapine. The V118I/T215Y mutant was not replication impaired; whereas H208Y/T215Y and V118I/H208Y/T215Y had significantly (P < 0.01) reduced replication capacities of 40 and 35% of wild-type, respectively.

CONCLUSION

Different combinations of V118I, H208Y, and T215Y produce NNRTI hypersusceptibility. The V118I/T215Y mutant is hypersusceptible to delavirdine and nevirapine without reduced replication capacity, whereas the H208Y/T215Y and V118I/H208Y/T215Y mutants are hypersusceptible to all NNRTI and show impaired replication. These findings suggest that more than one mechanism is involved in NNRTI hypersusceptibility.

摘要

背景

HIV-1对非核苷类逆转录酶抑制剂（NNRTI）的超敏感性可改善含NNRTI方案的疗效。在我们早期对来自接受过治疗的患者的病毒分离株配对基因型-表型数据集的分析中，部分确定了NNRTI超敏感性的遗传基础，其中我们鉴定出逆转录酶突变V118I、H208Y和T215Y与NNRTI超敏感性密切相关。

目的

我们通过定点诱变和HIV-1重组体的表型分析评估了这些突变在NNRTI超敏感性中的作用。

方法

在单循环试验中测定药物敏感性和复制能力。超敏感性定义为50%抑制浓度（IC50）的平均变化倍数具有统计学意义（P < 0.01；学生t检验）且小于0.4。

结果

单个突变V118I、H208Y和T215Y对依非韦伦未显示超敏感性，平均变化倍数分别为0.58、0.55和0.70（P < 0.01和P = 0.12）。H208Y/T215Y和V118I/H208Y/T215Y突变体对依非韦伦显示出明显的超敏感性，平均变化倍数分别为0.27和0.20（P < 0.001）。此外，H208Y/T215Y、V118I/T215Y和V118I/H208Y/T215Y对地拉韦啶和奈韦拉平超敏感。V118I/T215Y突变体的复制未受损；而H208Y/T215Y和V118I/H208Y/T215Y的复制能力分别显著降低（P < 0.01）至野生型的40%和35%。