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缺氧诱导内皮细胞Weibel-Palade小体的胞吐作用。一种心脏保存后快速募集中性粒细胞的机制。

Hypoxia-induced exocytosis of endothelial cell Weibel-Palade bodies. A mechanism for rapid neutrophil recruitment after cardiac preservation.

作者信息

Pinsky D J, Naka Y, Liao H, Oz M C, Wagner D D, Mayadas T N, Johnson R C, Hynes R O, Heath M, Lawson C A, Stern D M

机构信息

Department of Medicine, Columbia University College of Physicians and Surgeons, New York 10032, USA.

出版信息

J Clin Invest. 1996 Jan 15;97(2):493-500. doi: 10.1172/JCI118440.

Abstract

The period of hypoxia is an important priming event for the vascular dysfunction that accompanies reperfusion, with endothelial cells (ECs) and neutrophils (PMNs) playing a central role. We hypothesized that EC Weibel-Palade (WP) body exocytosis during the hypoxic/ischemic period during organ preservation permits brisk PMN recruitment into postischemic tissue, a process further amplified in an oxidant-rich milieu. Exposure of human umbilical vein ECs to a hypoxic environment (pO2 approximately 20 torr) stimulated release of von Willebrand factor (vWF), stored in EC WP bodies, as well as increased expression of the WP body-derived PMN adhesion molecule P-selectin at the EC surface. Increased binding of 111In-labeled PMNs to hypoxic EC monolayers (compared with normoxic controls) was blocked with a blocking antibody to P-selectin, but was not affected by a nonblocking control antibody. Although increased P-selectin expression and vWF release were also noted during reoxygenation, hypoxia alone (even in the presence of antioxidants) was sufficient to increase WP body exocytosis. To determine the relevance of these observations to hypothermic cardiac preservation, during which the pO2 within the cardiac vasculature declines to similarly low levels, experiments were performed in a rodent (rat and mouse) cardiac preservation/transplantation model. Immunodepletion of recipient PMNs or administration of a blocking anti-P-selectin antibody before transplantation resulted in reduced graft neutrophil infiltration and improved graft survival, compared with identically preserved hearts transplanted into control recipients. To establish the important role of endothelial P-selectin expression on the donor vasculature, murine cardiac transplants were performed using homozygous P-selectin deficient and wild-type control donor hearts flushed free of blood/platelets before preservation/transplantation. P-selectin-null hearts transplanted into wild-type recipients demonstrated a marked (13-fold) reduction in graft neutrophil infiltration and increased graft survival compared with wild-type hearts transplanted into wild-type recipients. To determine whether coronary endothelial WP exocytosis may occur during cardiac preservation in humans, the release of vWF into the coronary sinus (CS) was measured in 32 patients during open heart surgery. CS samples obtained at the start and conclusion of the ischemic period demonstrated an increase in CS vWF antigen (by ELISA) consisting of predominantly high molecular weight multimers (by immunoelectrophoresis). These data suggest that EC WP exocytosis occurs during hypothermic cardiac preservation, priming the vasculature to recruit PMNs rapidly during reperfusion.

摘要

缺氧期是伴随再灌注的血管功能障碍的一个重要引发事件,其中内皮细胞(ECs)和中性粒细胞(PMNs)起核心作用。我们假设,在器官保存的缺氧/缺血期,ECs的Weibel-Palade(WP)小体胞吐作用可使PMN迅速募集到缺血后组织中,这一过程在富含氧化剂的环境中会进一步放大。将人脐静脉ECs暴露于低氧环境(pO2约20托)会刺激储存于EC WP小体中的血管性血友病因子(vWF)释放,同时EC表面源自WP小体的PMN黏附分子P-选择素的表达也会增加。与常氧对照组相比,111In标记的PMN与缺氧EC单层的结合增加,而这种增加可被P-选择素阻断抗体阻断,但不受非阻断对照抗体影响。尽管在复氧过程中也观察到P-选择素表达增加和vWF释放,但仅缺氧(即使存在抗氧化剂)就足以增加WP小体胞吐作用。为了确定这些观察结果与低温心脏保存的相关性(在此期间心脏血管内的pO2会降至类似的低水平),在啮齿动物(大鼠和小鼠)心脏保存/移植模型中进行了实验。与移植到对照受体的同等保存的心脏相比,在移植前对受体PMN进行免疫清除或给予P-选择素阻断抗体可减少移植物中性粒细胞浸润并提高移植物存活率。为了确定内皮P-选择素表达在供体血管上的重要作用,在保存/移植前将无血/无血小板冲洗的纯合P-选择素缺陷型和野生型对照供体心脏用于小鼠心脏移植。与移植到野生型受体的野生型心脏相比,移植到野生型受体的P-选择素缺失心脏的移植物中性粒细胞浸润显著减少(13倍),移植物存活率提高。为了确定人类心脏保存期间冠状动脉内皮WP小体胞吐作用是否会发生,在32例心脏直视手术患者中测量了冠状动脉窦(CS)中vWF的释放。在缺血期开始和结束时采集的CS样本显示,CS中vWF抗原增加(通过ELISA法),主要由高分子量多聚体组成(通过免疫电泳法)。这些数据表明,EC WP小体胞吐作用在低温心脏保存期间发生,使血管系统在再灌注期间迅速募集PMN。

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