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在一名接受高效抗逆转录病毒治疗(HAART)出现周期性变化的患者中,药物诱导HIV-1准种发生区室化的分子证据。

Molecular evidence for drug-induced compartmentalization of HIV-1 quasispecies in a patient with periodic changes to HAART.

作者信息

Wang Y M, Dyer W B, Workman C, Wang B, Sullivan J S, Saksena N K

机构信息

Retroviral Genetics Laboratory, Centre for Virus Research, Westmead Millennium Institutes, Westmead Hospital, NSW, Sydney, Australia.

出版信息

AIDS. 2000 Oct 20;14(15):2265-72. doi: 10.1097/00002030-200010200-00007.

Abstract

OBJECTIVE

To perform molecular analysis of the predominant viral populations and drug-resistance mutations from plasma and peripheral blood mononuclear cell (PBMC) compartments over time from an HIV infected patient, who experienced virological failure while on different HAART regimens.

MATERIALS AND METHODS

In a longitudinal study proviral and plasma HIV-1 sequences were amplified in the pol, protease and env genes and were sequenced directly and analysed phylogenetically. Virus was recovered from time points corresponding to viral load peaks using co-culturing techniques. The periodic failure of different highly active antiretroviral therapy (HAART) regimens was analysed sequencing.

RESULTS

Longitudinal follow-up studies revealed four inflection peaks of plasma viraemia associated with the recovery of culturable virus in vitro, which indicated failure of the concurrent HAART regimen. Molecular analysis of viral strains revealed evidence of continual evolution and compartmentalization of drug-resistance mutants/quasispecies between plasma and PBMC, with the widest spectrum of mutations isolated from plasma. Importantly, these data show the periodic appearance and clearance of drug-resistance mutants concomitant with the introduction and withdrawal of zidovudine over time.

CONCLUSION

This report is unique in showing drug-induced compartmentalization of viral quasispecies under the control of different HAART regimens in both plasma and PBMC. Introduction and withdrawal of zidovudine from the HAART regimen had direct bearing on the appearance and disappearance of specific zidovudine drug-resistance mutations in plasma-derived virus. This data has important implications for the management of HIV-infected patients with poor compliance with certain HAART regimens, and also in predicting the late emergence of drug-resistance mutations via the latent integrated provirus.

摘要

目的

对一名感染HIV的患者在不同高效抗逆转录病毒治疗(HAART)方案下随时间推移血浆和外周血单个核细胞(PBMC)区室中主要病毒群体和耐药突变进行分子分析,该患者在治疗期间出现病毒学失败。

材料和方法

在一项纵向研究中,对前病毒和血浆HIV-1序列在pol、蛋白酶和env基因中进行扩增,直接测序并进行系统发育分析。使用共培养技术从与病毒载量峰值对应的时间点回收病毒。对不同高效抗逆转录病毒治疗(HAART)方案的周期性失败进行测序分析。

结果

纵向随访研究揭示了血浆病毒血症的四个拐点峰值,与体外可培养病毒的恢复相关,这表明同时进行的HAART方案失败。病毒株的分子分析显示了耐药突变体/准种在血浆和PBMC之间持续进化和区室化的证据,从血浆中分离出的突变谱最广。重要的是,这些数据显示了随着时间的推移,耐药突变体随着齐多夫定的引入和停用而周期性出现和清除。

结论

本报告独特之处在于展示了在不同HAART方案控制下,血浆和PBMC中病毒准种的药物诱导区室化。在HAART方案中引入和停用齐多夫定与血浆来源病毒中特定齐多夫定耐药突变的出现和消失直接相关。这些数据对于管理依从性差的HIV感染患者以及预测通过潜伏整合前病毒导致的耐药突变的晚期出现具有重要意义。

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