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大鼠微循环中的小动脉收缩与局部肾素-血管紧张素系统

Arteriolar constriction and local renin-angiotensin system in rat microcirculation.

作者信息

Vicaut E, Hou X

机构信息

Laboratoire de Biophysique, Hôpital F. Widal, Paris, France.

出版信息

Hypertension. 1993 Apr;21(4):491-7. doi: 10.1161/01.hyp.21.4.491.

Abstract

Intravital microscopy was used in a preparation of rat cremaster muscle that was isolated from its normal blood supply and externally perfused with a physiological solution, thus allowing exclusion of circulating converting enzyme, renin, and angiotensinogen. The arterioles studied were classified as second-, third-, and fourth-order arterioles with mean diameters of 60.5, 29.9, and 14.8 microns, respectively. Topical administration of 1 nmol/mL angiotensin I or 1 nmol/mL tetradecapeptide renin substrate induced marked vasoconstrictions (i.e., 38.5%, 61.5%, and 90.1% and 25%, 34%, and 88% for second-, third-, and fourth-order arterioles with angiotensin I and tetradecapeptide renin substrate, respectively). The angiotensin converting enzyme inhibitor quinapril significantly inhibited the vasoconstrictions caused by either angiotensin I or tetradecapeptide renin substrate. Almost no vasoconstriction was found when angiotensinogen-rich renin-free plasma containing either 2.45 nmol/mL of angiotensinogen or 1.2 micrograms/mL renin was administered. Conversely, these two compounds induced significant constrictions in cremaster muscle preparations in which normal blood perfusion (and thus circulating renin and angiotensinogen) was left in place. We concluded that, in skeletal muscle, 1) the microvascular network is a very effective site of local angiotensin converting enzyme activity and consequently an important target site of angiotensin converting enzyme inhibitors; 2) the effects of tetradecapeptide renin substrate are very different from those of angiotensinogen from plasma and suggest that a large part of the effect of tetradecapeptide renin substrate was due to its nonspecific hydrolysis; and 3) at the microvascular level, circulating renin and angiotensinogen are more effective in inducing arteriolar constriction, in the presence of their substrate or associated enzyme, than local renin and angiotensinogen.

摘要

在大鼠提睾肌制备物中采用活体显微镜检查,该提睾肌与其正常血液供应分离,并外用生理溶液灌注,从而排除循环中的转化酶、肾素和血管紧张素原。所研究的小动脉分为二级、三级和四级小动脉,平均直径分别为60.5、29.9和14.8微米。局部给予1 nmol/mL血管紧张素I或1 nmol/mL十四肽肾素底物可引起明显的血管收缩(即,对于二级、三级和四级小动脉,血管紧张素I分别引起38.5%、61.5%和90.1%的收缩,十四肽肾素底物分别引起25%、34%和88%的收缩)。血管紧张素转化酶抑制剂喹那普利显著抑制血管紧张素I或十四肽肾素底物引起的血管收缩。当给予含有2.45 nmol/mL血管紧张素原或1.2微克/mL肾素的富含血管紧张素原的无肾素血浆时,几乎未发现血管收缩。相反,如果保留正常血液灌注(以及循环中的肾素和血管紧张素原),这两种化合物在提睾肌制备物中可引起显著收缩。我们得出结论:1) 在骨骼肌中,微血管网络是局部血管紧张素转化酶活性的一个非常有效的部位,因此是血管紧张素转化酶抑制剂的一个重要靶位点;2)十四肽肾素底物的作用与血浆血管紧张素原的作用非常不同,这表明十四肽肾素底物的大部分作用是由于其非特异性水解;3) 在微血管水平,在存在底物或相关酶的情况下,循环中的肾素和血管紧张素原比局部肾素和血管紧张素原在诱导小动脉收缩方面更有效。

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