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硫酸化聚甘露糖醛酸古罗糖醛酸,一种新型抗艾滋病候选药物,通过对抗线粒体的氧化损伤来抑制T细胞凋亡。

Sulfated polymannuroguluronate, a novel anti-AIDS drug candidate, inhibits T cell apoptosis by combating oxidative damage of mitochondria.

作者信息

Miao Benchun, Li Jing, Fu Xueyan, Gan Li, Xin Xianliang, Geng Meiyu

机构信息

Department of Pharmacology, Marine Drug and Food Institute, Ocean University of China, Qingdao 266003, People's Republic of China.

出版信息

Mol Pharmacol. 2005 Dec;68(6):1716-27. doi: 10.1124/mol.105.015412. Epub 2005 Sep 1.

Abstract

Sulfated polymannuroguluronate (SPMG) has entered the phase II clinical trial as the first anti-AIDS drug candidate in China. Herein, we report that SPMG was effective at protecting T lymphocytes against apoptosis. Further studies indicated that SPMG significantly elevated mitochondrial membrane potential (MMP) of T cells; inhibited mitochondrial release of cytochrome c (cyto c) in T cells; enhanced the activities of mitochondrial enzyme complex I, III, and V; and subsequently increased ATP level and ATP/ADP ratio. In addition, SPMG potently suppressed reactive oxygen species (ROS) generation in mitochondria at cellular level and scavenged free radicals in cell-free system. The molecular mechanism underlying the ATP-involved and ROS-dependent antiapoptosis of SPMG is characterized as having been caused by its engagement with mitochondrial import receptor and ADP/ATP carrier in T-cell outer and inner mitochondrial membrane, respectively. All these might shed new light on the understanding of anti-AIDS functions of SPMG by protecting T cells of persons infected with human immunodeficiency virus.

摘要

硫酸化聚甘露糖醛酸古洛糖醛酸(SPMG)作为中国首个抗艾滋病候选药物已进入二期临床试验。在此,我们报告SPMG在保护T淋巴细胞免受凋亡方面是有效的。进一步研究表明,SPMG显著提高了T细胞的线粒体膜电位(MMP);抑制了T细胞中线粒体细胞色素c(cyto c)的释放;增强了线粒体酶复合物I、III和V的活性;随后提高了ATP水平和ATP/ADP比率。此外,SPMG在细胞水平上有效抑制线粒体中活性氧(ROS)的产生,并在无细胞系统中清除自由基。SPMG涉及ATP和依赖ROS的抗凋亡分子机制的特征在于,它分别与T细胞线粒体外膜和内膜中的线粒体导入受体和ADP/ATP载体结合。所有这些可能为通过保护人类免疫缺陷病毒感染者的T细胞来理解SPMG的抗艾滋病功能提供新的线索。

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