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核苷类似物的线粒体毒性:机制、监测与管理

Mitochondrial toxicity of nucleoside analogues: mechanism, monitoring and management.

作者信息

Cherry Catherine L, Lala Luxshimi, Wesselingh Steven L

机构信息

Burnet Institute for Medical Research and Public Health, GPO Box 2284, Melbourne, Vic. 3001, Australia.

出版信息

Sex Health. 2005;2(1):1-11. doi: 10.1071/sh04016.

Abstract

Nucleoside analogues (NRTIs) are potent antiretroviral medications and are central to effective highly active antiretroviral therapy (HAART). Their intended action is to inhibit HIV reverse transcriptase. Nucleoside analogues also inhibit replication of mitochondrial DNA, and the pathogenesis of many of the toxicities associated with HAART is thought to be NRTI-induced mitochondrial dysfunction. Individuals with HIV infection may be particularly susceptible to clinically significant mitochondrial toxicity due to possible effects of HIV itself on mitochondria. At present there is no reliable method of detecting subclinical mitochondrial toxicity in patients exposed to NRTIs. Clinical awareness of this problem is therefore important to ensure the early detection of significant side effects and to allow timely consideration of changing therapy in those affected. There is no proven, effective therapy for NRTI-associated mitochondrial toxicity other than ceasing the implicated agent, and even with this strategy, resolution of symptoms may be incomplete. Similarly, there are no established methods for preventing mitochondrial toxicity in those on therapy including NRTIs. Micronutrients may have a role, but further study is needed to clarify optimal prevention as well as monitoring strategies.

摘要

核苷类似物(NRTIs)是强效抗逆转录病毒药物,是有效的高效抗逆转录病毒疗法(HAART)的核心。其预期作用是抑制HIV逆转录酶。核苷类似物还抑制线粒体DNA的复制,许多与HAART相关的毒性的发病机制被认为是由NRTI引起的线粒体功能障碍。由于HIV本身可能对线粒体产生影响,HIV感染者可能对具有临床意义的线粒体毒性特别敏感。目前,没有可靠的方法来检测接触NRTIs的患者的亚临床线粒体毒性。因此,临床意识到这个问题对于确保早期发现严重副作用以及及时考虑对受影响者改变治疗方法很重要。除了停用相关药物外,没有经过验证的有效治疗NRTI相关线粒体毒性的方法,即使采用这种策略,症状的缓解也可能不完全。同样,对于接受包括NRTIs在内的治疗的患者,也没有既定的预防线粒体毒性的方法。微量营养素可能起作用,但需要进一步研究以明确最佳预防措施以及监测策略。

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