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胰岛素对大鼠迷走神经背核复合体的胃运动及心血管效应

Gastric motor and cardiovascular effects of insulin in dorsal vagal complex of the rat.

作者信息

Krowicki Z K, Nathan N A, Hornby P J

机构信息

Department of Pharmacology and Experimental Therapeutics, Louisiana State University Medical Center, New Orleans, Louisiana 70112, USA.

出版信息

Am J Physiol. 1998 Nov;275(5):G964-72. doi: 10.1152/ajpgi.1998.275.5.G964.

Abstract

Insulin-binding sites exist in the lower brain stem of the rat, raising the possibility that the circulating hormone may have cardiovascular and gastric effects at this site. Therefore, we investigated the autonomic effects of applying rat insulin to the surface of the dorsal medulla (0.3 and 3 microU/rat) or microinjecting it into the dorsal vagal complex (DVC) (0.1-10 nU/site) in anesthetized rats. Application of rat insulin to the surface (3 microU/rat) and its microinjection into the DVC (1 and 10 nU/site) both evoked marked, albeit transient, increases in intragastric pressure, pyloric and greater curvature contractile activity, and blood pressure. Much higher doses of human (100 mU) and porcine insulin (3 mU) were needed to evoke modest changes in gastric motor and cardiovascular function when applied to the surface of the dorsal medulla. In addition, a 1,000-fold higher dose of porcine insulin (10 microU) in the DVC was not enough to mimic the autonomic effects of rat insulin microinjected into the same site. The excitatory gastric motor effects of rat insulin in the lower brain stem were abolished by vagotomy, whereas spinal cord transection blocked insulin-evoked increases in blood pressure. To test whether the gastric motor effects of rat insulin in the lower brain stem were caused by potential contamination with pancreatic polypeptide, we microinjected rat pancreatic polypeptide into the DVC at a single dose of 2 pmol. Only a modest increase in intragastric pressure in response to the hormone was observed. Thus it is likely that insulin, through its action in the lower brain stem, may be implicated in the pathogenesis of gastrointestinal and cardiovascular complications in hyperinsulinemia. In addition, species variations in the amino acid sequence of insulin may affect its biological activity in the brain of different species.

摘要

胰岛素结合位点存在于大鼠的低位脑干中,这增加了循环激素可能在此部位产生心血管和胃部效应的可能性。因此,我们研究了在麻醉大鼠中,将大鼠胰岛素应用于延髓背侧表面(0.3和3微单位/只大鼠)或将其微量注射到迷走神经背核(DVC)(0.1 - 10纳单位/部位)的自主神经效应。将大鼠胰岛素应用于表面(3微单位/只大鼠)及其微量注射到DVC(1和10纳单位/部位)均引起胃内压、幽门和胃大弯收缩活动以及血压显著但短暂的升高。当将更高剂量的人胰岛素(100毫单位)和猪胰岛素(3毫单位)应用于延髓背侧表面时,仅引起胃运动和心血管功能的适度变化。此外,在DVC中剂量高出1000倍的猪胰岛素(10微单位)不足以模拟微量注射到同一部位的大鼠胰岛素的自主神经效应。迷走神经切断术消除了大鼠胰岛素在低位脑干中的兴奋性胃运动效应,而脊髓横断则阻断了胰岛素引起的血压升高。为了测试大鼠胰岛素在低位脑干中的胃运动效应是否由潜在的胰多肽污染引起,我们以2皮摩尔的单剂量将大鼠胰多肽微量注射到DVC中。仅观察到对该激素的胃内压适度升高。因此,胰岛素可能通过其在低位脑干中的作用,参与高胰岛素血症时胃肠道和心血管并发症的发病机制。此外,胰岛素氨基酸序列的种属差异可能会影响其在不同物种大脑中的生物活性。

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