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巨大霉素抑制HIV-1复制并干扰gp160加工。

Megalomicin inhibits HIV-1 replication and interferes with gp160 processing.

作者信息

San José E, Muñoz-Fernández M A, Alarcón B

机构信息

Centro de Biología Molecular Severo Ochoa, CSIC-UAM, Universidad Autónoma de Madrid, Spain.

出版信息

Virology. 1997 Dec 22;239(2):303-14. doi: 10.1006/viro.1997.8872.

Abstract

The inhibitory effects on HIV replication of megalomicin (MGM, an inhibitor of intra-Golgi vesicle transport, have been studied. In experiments at low multiplicity of infection on Jurkat and MT2 cell lines. MGM inhibited the production of p24 antigen, the formation of syncytia, and the induction of apoptosis at concentrations below 5 microM. Furthermore, PCR analysis of genomic DNA showed that, in the presence of MGM, HIV-1 had been eradicated from the culture. MGM also inhibited replication of primary isolates of HIV-1 in blood lymphoblasts and more importantly, at 1 microM, MGM inhibited depletion of CD4+ T cells in cultures of blood lymphocytes from seropositive patients. Finally, MGM inhibited the generation of infectious virions and the processing of the envelope protein precursor gp160 to its mature forms, resulting in the rapid degradation of gp 160. These data suggest that MGM induces a powerful inhibitory effect on HIV-1 replication at nontoxic concentrations by preventing the processing of HIV-1 gp160 envelope protein and the subsequent formation of infectious viral particles.

摘要

巨球霉素(MGM,一种高尔基体内囊泡运输抑制剂)对HIV复制的抑制作用已得到研究。在对Jurkat和MT2细胞系进行低感染复数的实验中,MGM在浓度低于5微摩尔时可抑制p24抗原的产生、多核体的形成以及细胞凋亡的诱导。此外,对基因组DNA的PCR分析表明,在MGM存在的情况下,HIV-1已从培养物中被根除。MGM还抑制了HIV-1原代分离株在血液淋巴细胞中的复制,更重要的是,在1微摩尔时,MGM抑制了血清阳性患者血液淋巴细胞培养物中CD4 + T细胞的消耗。最后,MGM抑制了感染性病毒粒子的产生以及包膜蛋白前体gp160向其成熟形式的加工,导致gp160迅速降解。这些数据表明,MGM通过阻止HIV-1 gp160包膜蛋白的加工以及随后感染性病毒颗粒的形成,在无毒浓度下对HIV-1复制产生强大的抑制作用。

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