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HIV在淋巴细胞中的复制动力学及蛋白酶抑制剂的疗效

Dynamics of HIV replication in lymphocytes and the efficacy of protease inhibitors.

作者信息

Bermejo Mercedes, Sánchez-Palomino Sonsoles, Usán Luis, Alcamí José

机构信息

AIDS Immunopathogenesis Unit, Centro Nacional de Microbiología, Instituto de Salud Carlos III, Madrid, Spain.

出版信息

J Med Virol. 2004 Aug;73(4):502-7. doi: 10.1002/jmv.20118.

Abstract

Using a system that allows transfection of resting peripheral blood lymphocytes (PBLs) two questions were addressed: the kinetics of HIV replication from the state of proviral latency, and the impact of different parameters on the efficacy of protease inhibitors to control HIV replication. PBLs were transfected with an infectious full length HIV-DNA harboring a luciferase reporter gene and activated thereafter. Ritonavir was added at different times at doses ranging from to 0.06 to 1 microM. Viral expression was assessed by quantifying luciferase activity in cell extracts and levels of p24 HIV antigen in culture supernatants. After transfection and cell activation, intracellular expression of HIV proteins, as assessed by luciferase detection, occurred within 2 hr. HIV-gag p24 antigen was detected in culture supernatants between 6 and 8 hr post-activation. Ritonavir was effective in blocking viral replication when given within 4 hr following HIV reactivation, but a delay in ritonavir administration or breaches in ritonavir levels after 6 hr from transfection resulted in viral escape. HIV reactivation from proviral latency in PBLs is an extremely rapid process, faster than estimated from previous models. These data stress the need for maintaining effective antiretroviral concentrations to block completely viral replication.

摘要

利用一个允许转染静息外周血淋巴细胞(PBLs)的系统,研究了两个问题:从原病毒潜伏状态开始的HIV复制动力学,以及不同参数对蛋白酶抑制剂控制HIV复制效力的影响。用携带荧光素酶报告基因的感染性全长HIV-DNA转染PBLs,然后激活这些细胞。在不同时间以0.06至1微摩尔的剂量添加利托那韦。通过定量细胞提取物中的荧光素酶活性和培养上清液中p24 HIV抗原的水平来评估病毒表达。转染和细胞激活后,通过荧光素酶检测评估,HIV蛋白的细胞内表达在2小时内发生。激活后6至8小时在培养上清液中检测到HIV-gag p24抗原。在HIV重新激活后4小时内给予利托那韦可有效阻断病毒复制,但利托那韦给药延迟或转染后6小时后利托那韦水平出现波动会导致病毒逃逸。PBLs中原病毒潜伏状态下的HIV重新激活是一个极其快速的过程,比之前模型估计的要快。这些数据强调了维持有效的抗逆转录病毒浓度以完全阻断病毒复制的必要性。

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