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组胺对大鼠胃微血管通透性的影响。

Effect of histamine on microvascular permeability in the rat stomach.

作者信息

Nagata H, Guth P H

出版信息

Am J Physiol. 1983 Aug;245(2):G201-7. doi: 10.1152/ajpgi.1983.245.2.G201.

Abstract

The effect of histamine on gastric microvascular permeability to macromolecules in the rat was studied using fluorescent in vivo microscopy. Histamine was applied topically to the serosal surface for study of the muscularis externa, to the submucosa, and to the superficial mucosa, and the area of leaks of a fluorescein-albumin conjugate from microvessels was quantitated. In the muscularis externa both histamine and an H1-agonist, but not an H2-agonist, caused dose-dependent leak of conjugate from venules. An H1-antagonist, but not an H2-antagonist, decreased the histamine-induced leak. In the submucosa histamine caused dose-dependent dilatation of arterioles but not leak of conjugate. In contrast, bradykinin caused both dose-dependent dilatation of arterioles and leak of conjugate from venules. In the superficial mucosa histamine did not cause any leak. In conclusion, topical histamine 1) increased microvascular permeability to macromolecules from venules in the muscularis externa via H1-receptors, 2) did not affect microvascular permeability in the submucosa (this may be due to lack of histamine receptors on the venules as bradykinin increased venular permeability), and 3) did not affect microvascular permeability in the superficial mucosa, but there might not have been adequate histamine backdiffusion.

摘要

利用荧光体内显微镜技术研究了组胺对大鼠胃微血管大分子通透性的影响。将组胺局部应用于浆膜表面以研究外肌层、黏膜下层和浅表黏膜,对微血管中荧光素 - 白蛋白偶联物的渗漏面积进行定量。在外肌层,组胺和H1激动剂均可引起小静脉中偶联物的剂量依赖性渗漏,而H2激动剂则无此作用。H1拮抗剂可减少组胺诱导的渗漏,而H2拮抗剂则无此作用。在黏膜下层,组胺引起小动脉的剂量依赖性扩张,但不引起偶联物渗漏。相比之下,缓激肽既引起小动脉的剂量依赖性扩张,又引起小静脉中偶联物的渗漏。在浅表黏膜中,组胺未引起任何渗漏。总之,局部应用组胺:1)通过H1受体增加外肌层小静脉对大分子的微血管通透性;2)不影响黏膜下层的微血管通透性(这可能是由于小静脉上缺乏组胺受体,因为缓激肽可增加小静脉通透性);3)不影响浅表黏膜的微血管通透性,但可能没有足够的组胺反向扩散。

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