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修饰血红蛋白可在大鼠肠系膜中产生小静脉内皮间隙并导致白蛋白渗漏。

Modified hemoglobins produce venular interendothelial gaps and albumin leakage in the rat mesentery.

作者信息

Baldwin A L

机构信息

Department of Physiology, College of Medicine, University of Arizona, Tucson, Arizona 85724-5051, USA.

出版信息

Am J Physiol. 1999 Aug;277(2):H650-9. doi: 10.1152/ajpheart.1999.277.2.H650.

Abstract

Cross-linked hemoglobin (alphaalpha-Hb) and polyethylene glycol (PEG)-conjugated Hb have both been considered as possible "blood substitutes." Previously, we showed that PEG-Hb extravasates rapidly in the intestinal mucosa and causes transient epithelial sloughing, resulting in temporary opening of the intestinal epithelial barrier. In the present study, the rat mesenteric preparation was used to quantify the effects of the two Hbs on microvascular leakage to albumin and to investigate possible changes in the integrity of the interendothelial cell junctions and the endothelial actin cytoskeleton. In anesthetized Sprague-Dawley rats, the microvasculature of a mesenteric window was perfused with HEPES-buffered saline (HBS) containing 0.5 mg/ml BSA and 2 mg/ml alphaalpha-Hb (n = 16) or PEG-Hb (n = 5) for 2 or 10 min. Controls (n = 4) just received HBS-BSA. In some experiments (n = 9 for alphaalpha-Hb; n = 5 for PEG-Hb), the perfusate was then replaced by FITC-albumin in HBS-BSA for the next 3 min. The vasculature was then perfusion fixed, stained for filamentous actin and for mast cells, and viewed microscopically. In the remaining experiments, the mesenteric microvasculature was stained with silver nitrate to determine the number of endothelial junctional gaps per length of venules. Both Hbs increased the number and area of leaks per micrometer of venular length compared with control, but alphaalpha-Hb increased to a greater extent than PEG-Hb. Formation of leaks was accompanied by changes in the endothelial actin cytoskeleton and by an increased number of endothelial gaps. Mast cell degranulation was significantly greater (P < 0.05) in Hb-treated preparations compared with controls, but there was no direct correlation between sites of degranulation and albumin leakage. These Hbs appear to induce venular leakage in the mesentery by mechanisms similar to those previously observed after treatment with histamine or nitric oxide synthase inhibitors.

摘要

交联血红蛋白(αα-Hb)和聚乙二醇(PEG)共轭血红蛋白都曾被视为可能的“血液替代品”。此前,我们发现PEG-Hb在肠黏膜中迅速渗出,导致上皮细胞短暂脱落,致使肠上皮屏障暂时开放。在本研究中,使用大鼠肠系膜制剂来量化这两种血红蛋白对白蛋白微血管渗漏的影响,并研究内皮细胞间连接和内皮肌动蛋白细胞骨架完整性可能发生的变化。在麻醉的Sprague-Dawley大鼠中,用含有0.5mg/ml牛血清白蛋白(BSA)和2mg/mlαα-Hb(n = 16)或PEG-Hb(n = 5)的HEPES缓冲盐水(HBS)灌注肠系膜窗的微血管2或10分钟。对照组(n = 4)仅接受HBS-BSA。在一些实验中(αα-Hb组n = 9;PEG-Hb组n = 5),随后在接下来的3分钟内用HBS-BSA中的异硫氰酸荧光素(FITC)标记的白蛋白替换灌注液。然后对血管进行灌注固定,用丝状肌动蛋白和肥大细胞染色,并进行显微镜观察。在其余实验中,用硝酸银对肠系膜微血管进行染色,以确定每单位长度小静脉的内皮连接间隙数量。与对照组相比,两种血红蛋白均增加了每微米小静脉长度的渗漏数量和面积,但αα-Hb的增加幅度大于PEG-Hb。渗漏的形成伴随着内皮肌动蛋白细胞骨架的变化以及内皮间隙数量的增加。与对照组相比,血红蛋白处理组的肥大细胞脱颗粒明显更严重(P < 0.05),但脱颗粒部位与白蛋白渗漏之间无直接相关性。这些血红蛋白似乎通过与先前用组胺或一氧化氮合酶抑制剂处理后观察到的机制类似的机制诱导肠系膜小静脉渗漏。

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