与核苷类逆转录酶抑制剂治疗相关的脂肪细胞线粒体DNA耗竭及形态学改变。
Mitochondrial DNA depletion and morphologic changes in adipocytes associated with nucleoside reverse transcriptase inhibitor therapy.
作者信息
Nolan David, Hammond Emma, Martin Annalise, Taylor Louise, Herrmann Susan, McKinnon Elizabeth, Metcalf Cecily, Latham Bruce, Mallal Simon
机构信息
Centre for Clinical Immunology and Biomedical Statistics, Royal Perth Hospital and Murdoch University, Western Australia, Australia.
出版信息
AIDS. 2003 Jun 13;17(9):1329-38. doi: 10.1097/00002030-200306130-00007.
BACKGROUND
Nucleoside analogue reverse transcriptase inhibitor (NRTI) therapy provides sufficient conditions for progressive subcutaneous fat wasting in HIV-infected patients. As NRTI-induced host toxicity is proposed to involve cellular mitochondrial DNA (mtDNA) depletion, determinants of cellular mtDNA copy number and mitochondrial mass in adipocyte samples from NRTI-treated HIV-infected patients and antiretroviral-naive controls were investigated. Adipose tissue morphology was also assessed.
METHODS
Subcutaneous fat samples were obtained from NRTI-treated, HIV-infected patients (n = 21), antiretroviral therapy-naive HIV-infected controls (n = 11), and HIV-seronegative controls (n = 6). Non-adipocytes were removed by collagenase digestion. Adipocyte mtDNA copies/cell was measured using a real time PCR-based assay, and adipocyte mitochondrial protein content was also measured. Light and electron microscopy were performed on tissue samples.
FINDINGS
Adipocyte mtDNA copies/cell values were similar (P = 0.56) in HIV seronegative and HIV-infected control groups. NRTI treatment was associated with reduced adipocyte mtDNA copies/cell, representing mean mtDNA depletion in NRTI-treated individuals of 77.7% compared with the mean value for the HIV-infected control group (P < 0001). Additionally, significant differences were found in adipocyte mtDNA copies/cell between patients receiving stavudine (n = 12, mean mtDNA depletion 87.1%) and zidovudine (n = 9, mean mtDNA depletion 52.1%) (P < 0.001). Adipocyte mitochondrial mass was increased in the stavudine group only (mean increase 289%, P < 0.01).
INTERPRETATION
NRTI therapy is associated with mtDNA depletion and mitochondrial proliferation in adipocytes, consistent with the hypothesis that NRTI-induced mtDNA depletion contributes to the pathogenesis of subcutaneous fat wasting. Morphologic assessment also supports a role for NRTI therapy in inducing adipocyte metabolic dysfunction and cell death.
背景
核苷类似物逆转录酶抑制剂(NRTI)疗法为HIV感染患者进行性皮下脂肪消耗提供了充分条件。由于NRTI诱导的宿主毒性被认为与细胞线粒体DNA(mtDNA)耗竭有关,因此对接受NRTI治疗的HIV感染患者和未接受抗逆转录病毒治疗的对照者脂肪细胞样本中细胞mtDNA拷贝数和线粒体质量的决定因素进行了研究。同时也评估了脂肪组织形态。
方法
从接受NRTI治疗的HIV感染患者(n = 21)、未接受抗逆转录病毒治疗的HIV感染对照者(n = 11)和HIV血清阴性对照者(n = 6)获取皮下脂肪样本。通过胶原酶消化去除非脂肪细胞。使用基于实时PCR的检测方法测量脂肪细胞mtDNA拷贝数/细胞,并测量脂肪细胞线粒体蛋白含量。对组织样本进行光镜和电镜检查。
结果
HIV血清阴性和HIV感染对照组的脂肪细胞mtDNA拷贝数/细胞值相似(P = 0.56)。NRTI治疗与脂肪细胞mtDNA拷贝数/细胞减少有关,与HIV感染对照组的平均值相比,接受NRTI治疗的个体mtDNA平均耗竭77.7%(P < 0.001)。此外,接受司他夫定治疗的患者(n = 12,平均mtDNA耗竭87.1%)和齐多夫定治疗的患者(n = 9,平均mtDNA耗竭52.1%)之间的脂肪细胞mtDNA拷贝数/细胞存在显著差异(P < 0.001)。仅司他夫定组的脂肪细胞线粒体质量增加(平均增加289%,P < 0.01)。
解读
NRTI治疗与脂肪细胞中的mtDNA耗竭和线粒体增殖有关,这与NRTI诱导的mtDNA耗竭导致皮下脂肪消耗发病机制的假设一致。形态学评估也支持NRTI治疗在诱导脂肪细胞代谢功能障碍和细胞死亡中起作用。
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