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HIV感染个体中线粒体DNA水平与当前治疗状态之间的组织特异性关联。

Tissue-specific associations between mitochondrial DNA levels and current treatment status in HIV-infected individuals.

作者信息

Cherry Catherine L, Nolan David, James Ian R, McKinnon Elizabeth J, Mallal Simon A, Gahan Michelle E, Lal Luxshimi, McArthur Justin C, Wesselingh Steven L

机构信息

Macfarlane Burnet Institute for Medical Research and Public Health, Melbourne, Australia.

出版信息

J Acquir Immune Defic Syndr. 2006 Aug 1;42(4):435-40. doi: 10.1097/01.qai.0000224974.67962.ce.

Abstract

BACKGROUND

Tissue mitochondrial DNA (mtDNA) levels have been proposed as a marker of nucleoside analouge reverse transcriptase inhibitor (NRTI) toxicity. However, clinical studies have yielded conflicting data regarding possible associations with mtDNA levels. This study examined mtDNA levels in matched samples of peripheral blood mononuclear cells (PBMCs) and subcutaneous fat from a large Australian cohort to examine treatment, clinical, and demographic associations with mtDNA depletion.

METHODS

mtDNA was quantified by real-time polymerase chain reaction. Results were compared across patient treatment and demographic details using linear mixed models.

RESULTS

One hundred sixty-three PBMCs and 161 fat samples were available from 61 individuals. Current NRTI exposure was the major determinant of mtDNA levels. Both ddI (didanosine) and d4T (stavudine) exposures were associated with mtDNA depletion in fat (P < or = 0.0001 vs. those not on NRTIs). DdI exposure (P = 0.003), but not d4T exposure (P = 0.5), was associated with mtDNA depletion in PBMCs. No association between patient demographics or time on current therapy and mtDNA was observed.

CONCLUSIONS

Current NRTI exposure is the major determinant of tissue mtDNA, but the precise determinants are tissue specific. Both ddI and d4T exposure are associated with fat mtDNA depletion, whereas ddI exposure was the only observed association with mtDNA depletion in PBMCs.

摘要

背景

组织线粒体DNA(mtDNA)水平已被提议作为核苷类似物逆转录酶抑制剂(NRTI)毒性的标志物。然而,临床研究关于其与mtDNA水平可能的关联得出了相互矛盾的数据。本研究检测了来自澳大利亚一个大型队列的外周血单核细胞(PBMC)和皮下脂肪匹配样本中的mtDNA水平,以研究与mtDNA耗竭相关的治疗、临床和人口统计学因素。

方法

通过实时聚合酶链反应对mtDNA进行定量。使用线性混合模型比较患者治疗和人口统计学细节的结果。

结果

从61名个体中获取了163份PBMC样本和161份脂肪样本。当前NRTI暴露是mtDNA水平的主要决定因素。ddI(去羟肌苷)和d4T(司他夫定)暴露均与脂肪中的mtDNA耗竭相关(与未使用NRTI的患者相比,P≤0.0001)。ddI暴露(P = 0.003)与PBMC中的mtDNA耗竭相关,但d4T暴露(P = 0.5)则不然。未观察到患者人口统计学因素或当前治疗时间与mtDNA之间存在关联。

结论

当前NRTI暴露是组织mtDNA的主要决定因素,但确切决定因素具有组织特异性。ddI和d4T暴露均与脂肪mtDNA耗竭相关,而ddI暴露是观察到的与PBMC中mtDNA耗竭的唯一关联。

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