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补体灭活抗原,葡萄球菌致病性的一个可能决定因素。

Decomplementation antigen, a possible determinant of staphylococcal pathogenicity.

作者信息

Bhakdi S, Muhly M

出版信息

Infect Immun. 1985 Jan;47(1):41-6. doi: 10.1128/iai.47.1.41-46.1985.

Abstract

We report the existence of an extracellular staphylococcal product, designated staphylococcal decomplementation antigen (DA), that causes rapid consumption of early-reacting complement components up to and including C5 in human serum. Complement activation occurs as a consequence of immune complex formation between DA and specific human immunoglobulin G antibodies and proceeds primarily via the classical pathway. The terminal components C7, C8, and C9 are not consumed during the process. Levels of DA production do not correlate with the expression of classical pathogenic factors, such as coagulase, clumping factor, protein A, or alpha-toxin. DA is a nondialyzable macromolecule eluting in a molecular-weight region of 70,000 to 120,000 on Sephacryl S-300 and displaying an apparent sedimentation coefficient of 3 to 4 S on sucrose density gradients. The molecule is remarkably stable and resists destruction upon boiling for 30 min or by treatment with pronase, lysostaphin, DNase, or RNase. We anticipate that DA protects staphylococci from complement attack through induction of abortive, complement-consuming reactions in the fluid phase.

摘要

我们报告了一种细胞外葡萄球菌产物的存在,该产物被命名为葡萄球菌补体灭活抗原(DA),它可导致人血清中早期反应性补体成分迅速消耗,直至并包括C5。补体激活是DA与特异性人免疫球蛋白G抗体之间形成免疫复合物的结果,主要通过经典途径进行。在此过程中,终末成分C7、C8和C9未被消耗。DA的产生水平与凝固酶、聚集因子、蛋白A或α-毒素等经典致病因子的表达无关。DA是一种不可透析的大分子,在Sephacryl S-300上于分子量70,000至120,000区域洗脱,在蔗糖密度梯度上显示出3至4 S的表观沉降系数。该分子非常稳定,煮沸30分钟或用链霉蛋白酶、溶葡萄球菌素、DNase或RNase处理后均能抵抗破坏。我们预计DA通过在液相中诱导流产性的、消耗补体的反应来保护葡萄球菌免受补体攻击。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d79e/261459/e18298651241/iai00118-0058-a.jpg

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