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肝硬化大鼠体内的血管活性肠肽:血流动力学效应及肠系膜动脉受体特征

Vasoactive intestinal peptide in cirrhotic rats: hemodynamic effects and mesenteric arterial receptor characteristics.

作者信息

Lee S S, Huang M, Ma Z, Rorstad O

机构信息

Liver Unit, University of Calgary, Alberta, Canada.

出版信息

Hepatology. 1996 May;23(5):1174-80. doi: 10.1002/hep.510230536.

Abstract

Vasoactive intestinal peptide (VIP) blood levels in cirrhosis are elevated, but its hemodynamic and receptor characteristics remain unclarified. We aimed to quantify VIP receptor characteristics in mesenteric arteries, plasma VIP concentration by radioimmunoassay (RIA), and the hemodynamic effects of VIP infusion in bile duct-ligated (BDL) cirrhotic and sham-operated control rats. Mesenteric arterial membranes were prepared by ultracentrifugation, and receptor characteristics were studied using 125I-labeled VIP as a radioligand. For the hemodynamic study, there were four groups: cirrhotic and sham-operated rats were infused with either VIP (50 ng/kg/min for 15 minutes) or equivolumic isotonic saline. Regional blood flows were measured in conscious rats with radioactive microspheres. Receptor studies showed high- and low-affinity binding sites for VIP, which had similar equilibrium dissociation constants (binding affinities) and receptor densities for both the cirrhotic and control rats. Plasma VIP concentrations were significantly elevated in the cirrhotic rats. In both cirrhotic and sham-operated rats, VIP infusion produced plasma levels approximately twofold to threefold increased over the basal levels observed in cirrhotic rats. In cirrhotic rats, VIP infusion did not affect any hemodynamic parameter, whereas in the sham-operated rats VIP infusion significantly increased the mesenteric visceral blood flow. These results show that the hyporesponsiveness to VIP in cirrhotic rats is not attributable to receptor downregulation, implying postreceptor alterations. This suggests that VIP may not play a major role in the maintenance of splanchnic hyperemia in cirrhosis.

摘要

肝硬化患者血管活性肠肽(VIP)的血水平升高,但其血流动力学和受体特性仍不明确。我们旨在量化肠系膜动脉中VIP受体的特性、通过放射免疫分析(RIA)测定血浆VIP浓度,并研究VIP输注对胆管结扎(BDL)肝硬化大鼠和假手术对照大鼠的血流动力学影响。通过超速离心制备肠系膜动脉膜,使用125I标记的VIP作为放射性配体研究受体特性。在血流动力学研究中,分为四组:对肝硬化大鼠和假手术大鼠分别输注VIP(50 ng/kg/min,持续15分钟)或等体积的等渗盐水。用放射性微球测量清醒大鼠的局部血流量。受体研究显示VIP存在高亲和力和低亲和力结合位点,肝硬化大鼠和对照大鼠的平衡解离常数(结合亲和力)和受体密度相似。肝硬化大鼠的血浆VIP浓度显著升高。在肝硬化大鼠和假手术大鼠中,VIP输注后血浆水平均比肝硬化大鼠的基础水平升高约2至3倍。在肝硬化大鼠中,VIP输注不影响任何血流动力学参数,而在假手术大鼠中,VIP输注显著增加肠系膜内脏血流量。这些结果表明,肝硬化大鼠对VIP反应性降低并非归因于受体下调,提示存在受体后改变。这表明VIP可能在肝硬化内脏充血的维持中不起主要作用。

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