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炭疽毒素:保护性抗原在平面磷脂双分子层中的通道形成活性。

Anthrax toxin: channel-forming activity of protective antigen in planar phospholipid bilayers.

作者信息

Blaustein R O, Koehler T M, Collier R J, Finkelstein A

机构信息

Department of Physiology, Albert Einstein College of Medicine, Bronx, NY 10461.

出版信息

Proc Natl Acad Sci U S A. 1989 Apr;86(7):2209-13. doi: 10.1073/pnas.86.7.2209.

Abstract

The three separate proteins that make up anthrax toxin--protective antigen (PA), edema factor (EF), and lethal factor (LF)--act in binary combinations to produce two distinct reactions in experimental animals: edema (PA + EF) and death (PA + LF). PA is believed to interact with a membrane receptor, and after proteolytic processing, to mediate endocytosis and subsequent translocation of EF or LF into the cytosol. PA can be separated, after mild trypsinolysis, into two fragments, PA65 (65 kDa) and PA20 (20 kDa). We demonstrate that trypsin-cleaved PA is capable of forming cation-selective channels in planar phospholipid bilayer membranes and that this activity is confined to the PA65 fragment; PA20, LF, and EF are devoid of channel-forming activity. These PA65 channels exhibit pH-dependent and voltage-dependent activity--a property reminiscent of the channels formed by the two-chain proteins diphtheria, tetanus, and botulinum toxins.

摘要

构成炭疽毒素的三种独立蛋白质——保护性抗原(PA)、水肿因子(EF)和致死因子(LF)——以二元组合的形式发挥作用,在实验动物中产生两种不同的反应:水肿(PA + EF)和死亡(PA + LF)。据信,PA与膜受体相互作用,经过蛋白水解处理后,介导EF或LF的内吞作用以及随后向细胞质的转运。经过温和的胰蛋白酶消化后,PA可分离成两个片段,PA65(65 kDa)和PA20(20 kDa)。我们证明,胰蛋白酶切割后的PA能够在平面磷脂双层膜中形成阳离子选择性通道,并且这种活性仅限于PA65片段;PA20、LF和EF没有通道形成活性。这些PA65通道表现出pH依赖性和电压依赖性活性——这一特性让人联想到由双链蛋白质白喉毒素、破伤风毒素和肉毒杆菌毒素形成的通道。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0c44/286881/1b531f2245dd/pnas00247-0097-a.jpg

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