CNRS FR 3636, Université Paris Descartes, Paris, France.
Microbiology and Infection Research Domain, Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho, Braga, Portugal.
J Clin Invest. 2018 Apr 2;128(4):1627-1640. doi: 10.1172/JCI95127. Epub 2018 Mar 19.
Apoptosis has been proposed as a key mechanism responsible for CD4+ T cell depletion and immune dysfunction during HIV infection. We demonstrated that Q-VD-OPH, a caspase inhibitor, inhibits spontaneous and activation-induced death of T cells from SIV-infected rhesus macaques (RMs). When administered during the acute phase of infection, Q-VD-OPH was associated with (a) reduced levels of T cell death, (b) preservation of CD4+/CD8+ T cell ratio in lymphoid organs and in the gut, (c) maintenance of memory CD4+ T cells, and (d) increased specific CD4+ T cell response associated with the expression of cytotoxic molecules. Although therapy was limited to the acute phase of infection, Q-VD-OPH-treated RMs showed lower levels of both viral load and cell-associated SIV DNA as compared with control SIV-infected RMs throughout the chronic phase of infection, and prevented the development of AIDS. Overall, our data demonstrate that Q-VD-OPH injection in SIV-infected RMs may represent an adjunctive therapeutic agent to control HIV infection and delaying disease progression to AIDS.
细胞凋亡被认为是 HIV 感染过程中导致 CD4+T 细胞耗竭和免疫功能障碍的关键机制。我们证明,Caspase 抑制剂 Q-VD-OPH 可抑制 SIV 感染恒河猴(RMs)的 T 细胞自发性和激活诱导性死亡。在感染急性期给予 Q-VD-OPH 治疗时,与对照组 SIV 感染的 RMs 相比,Q-VD-OPH 治疗的 RMs 表现出:(a)T 细胞死亡水平降低;(b)淋巴器官和肠道中 CD4+/CD8+T 细胞比例得到维持;(c)记忆性 CD4+T 细胞得到维持;(d)与细胞毒性分子表达相关的特异性 CD4+T 细胞反应增加。尽管治疗仅限于感染急性期,但 Q-VD-OPH 治疗的 RMs 在整个慢性感染期间与对照组 SIV 感染的 RMs 相比,病毒载量和细胞相关 SIV DNA 的水平均较低,并预防了 AIDS 的发展。总的来说,我们的数据表明,在 SIV 感染的 RMs 中注射 Q-VD-OPH 可能成为一种辅助治疗药物,用于控制 HIV 感染并延缓疾病进展为 AIDS。
