核苷类似物逆转录酶抑制剂疗法对从群体水平到细胞水平脂肪萎缩的影响。

Contribution of nucleoside-analogue reverse transcriptase inhibitor therapy to lipoatrophy from the population to the cellular level.

作者信息

Nolan David, Hammond Emma, James Ian, McKinnon Elizabeth, Mallal Simon

机构信息

Centre for Clinical Immunology and Biomedical Statistics, Royal Perth Hospital, Murdoch University, Western Australia.

出版信息

Antivir Ther. 2003 Dec;8(6):617-26.

PMID:14760896

Abstract

OBJECTIVES

It has been proposed that the contribution of nucleoside-analogue reverse transcriptase inhibitor (NRTI) therapy to subcutaneous fat wasting involves adipose tissue-specific mitochondrial DNA toxicity. We have investigated the relationships between NRTI therapy, adipocyte mitochondrial DNA content, evidence of toxicity in adipose tissue and fat wasting in Caucasian male Western Australian HIV Cohort study participants.

METHODS

Longitudinal mixed effects analysis of fat wasting was undertaken in individuals receiving initial stavudine- or zidovudine-containing highly active antiretroviral measurements). Adipocyte mitochondrial DNA (mtDNA) depletion was also assessed according to current NRTI therapy in 92 subcutaneous fat biopsies from 69 HIV-positive individuals and seven healthy controls, and results were correlated with fat wasting among a subset of patients with biopsy data receiving initial stavudine- or zidovudine-containing HAART (n = 22, 103 DEXA measurements). Confocal microscopy was performed in 22 obtained after initiating/switching NRTI therapy.

RESULTS

Stavudine therapy was associated with more severe adipocyte mitochondrial DNA depletion (P < 0.001) and fat wasting over time (P = 0.002) compared with zidovudine therapy in independent analyses. Among patients with concurrent biopsy and longitudinal DEXA data, fat wasting was associated with duration of NRTI therapy (P = 0.001) and adipocyte mtDNA copies/cell (P = 0.01). In this analysis, the significant association between choice of stavudine versus zidovudine and fat wasting (P = 0.03) was lost after adjustment for the effect of mtDNA depletion (P = 0.13). Confocal analysis provided direct evidence of a relationship between severity of adipose tissue toxicity and mitochondrial DNA depletion. No significant effects of HIV protease inhibitor therapy were detected in these analyses.

CONCLUSIONS

Severity of subcutaneous fat wasting is primarily determined by choice of NRTI therapy (stavudine versus zidovudine) and by duration of exposure to the relevant NRTI. At the cellular level, evidence is provided that this effect manifests through NRTI-induced mitochondrial DNA depletion.

摘要

目的

有人提出核苷类似物逆转录酶抑制剂（NRTI）疗法导致皮下脂肪消耗是因为其对脂肪组织特异性的线粒体DNA毒性作用。在西澳大利亚HIV队列研究的白人男性参与者中，我们研究了NRTI疗法、脂肪细胞线粒体DNA含量、脂肪组织中毒性证据以及脂肪消耗之间的关系。

方法

对接受含司他夫定或齐多夫定的初始高效抗逆转录病毒治疗的个体进行脂肪消耗的纵向混合效应分析。还根据当前的NRTI疗法，对69名HIV阳性个体和7名健康对照的92份皮下脂肪活检样本中的脂肪细胞线粒体DNA（mtDNA）耗竭情况进行了评估，并将结果与一部分有活检数据且接受含司他夫定或齐多夫定的初始高效抗逆转录病毒治疗（HAART）的患者（n = 22，103次双能X线吸收测定）的脂肪消耗情况进行关联分析。在开始/更换NRTI治疗后获取的22个样本中进行了共聚焦显微镜检查。

结果

在独立分析中，与齐多夫定疗法相比，司他夫定疗法与更严重的脂肪细胞线粒体DNA耗竭（P < 0.001）以及随时间推移更严重的脂肪消耗（P = 0.002）相关。在同时有活检和纵向双能X线吸收测定数据的患者中，脂肪消耗与NRTI治疗持续时间（P = 0.001）和脂肪细胞mtDNA拷贝数/细胞（P = 0.01）相关。在该分析中，调整mtDNA耗竭的影响后，司他夫定与齐多夫定的选择和脂肪消耗之间的显著关联（P = 0.03）不再显著（P = 0.13）。共聚焦分析提供了脂肪组织毒性严重程度与线粒体DNA耗竭之间关系的直接证据。在这些分析中未检测到HIV蛋白酶抑制剂疗法有显著影响。