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天然抗体和补体诱导的内皮完整性短暂扰动。

Transient perturbation of endothelial integrity induced by natural antibodies and complement.

作者信息

Saadi S, Platt J L

机构信息

Department of Surgery, Duke University, Durham, North Carolina 27710.

出版信息

J Exp Med. 1995 Jan 1;181(1):21-31. doi: 10.1084/jem.181.1.21.

Abstract

The barrier function of blood vessels is though to be regulated at least in part by endothelium. This concept is supported by the dramatic loss of barrier function occurring in the hyperacute rejection of vascularized grafts mediated by anti-endothelial cell (EC) antibodies and complement. In this process, the endothelium is not destroyed but instead loses the ability to retain blood cells and plasma proteins within capillaries. The noncytotoxic mechanism that allows this change in EC function has been unknown. Here we report that within 10 to 20 min of exposure to human xenoreactive natural antibodies and complement, porcine EC undergo alterations in cell shape and in the cytoskeleton that disrupt monolayer integrity and lead to formation of intercellular gaps. Gap formation is not associated with cell death but requires the complement complex C5b67. The gaps induced by anti-EC antibodies and complement are transient; gap closure requires formation of C5b-9 complexes on the cells and the rate of recovery depends on the release of cellular products into the medium. Preincubation of EC with dibutyryl cAMP (0.5 mM) prevents gap formation and disruption of the cytoskeleton caused by antibodies and complement. These results provide evidence that the integrity of endothelium is regulated by components of the complement system and suggest a mechanism that may explain the prominent loss of endothelial integrity seen in humoral immune responses.

摘要

血管的屏障功能被认为至少部分受内皮细胞调节。这一概念得到了由抗内皮细胞(EC)抗体和补体介导的血管化移植物超急性排斥反应中屏障功能急剧丧失的支持。在这个过程中,内皮细胞并未被破坏,而是失去了在毛细血管内保留血细胞和血浆蛋白的能力。导致EC功能发生这种变化的非细胞毒性机制一直未知。在此我们报告,猪EC在暴露于人类异种反应性天然抗体和补体后的10至20分钟内,细胞形状和细胞骨架会发生改变,这会破坏单层完整性并导致细胞间间隙形成。间隙形成与细胞死亡无关,但需要补体复合物C5b67。抗EC抗体和补体诱导的间隙是短暂的;间隙闭合需要在细胞上形成C5b - 9复合物,恢复速度取决于细胞产物释放到培养基中的情况。用二丁酰环磷腺苷(0.5 mM)对EC进行预孵育可防止由抗体和补体引起的间隙形成和细胞骨架破坏。这些结果提供了证据表明内皮细胞的完整性受补体系统成分调节,并提示了一种可能解释在体液免疫反应中所见内皮完整性显著丧失的机制。

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