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大鼠脑中循环胰多肽的饱和结合位点特性研究

Characterization of saturable binding sites for circulating pancreatic polypeptide in rat brain.

作者信息

Whitcomb D C, Taylor I L, Vigna S R

机构信息

Department of Medicine, Duke University Medical Center, Durham, North Carolina 27710.

出版信息

Am J Physiol. 1990 Oct;259(4 Pt 1):G687-91. doi: 10.1152/ajpgi.1990.259.4.G687.

DOI:10.1152/ajpgi.1990.259.4.G687
PMID:2221079
Abstract

Pancreatic polypeptide (PP) inhibits pancreatic exocrine secretion by indirect mechanisms that may be centrally mediated. The central site of action of PP that results in inhibition of pancreatic secretion has not been identified. Using autoradiography to identify 125I-PP binding to frozen sections of rat brain, we have identified saturable, high-affinity PP receptors in high concentrations in the interpenduncular nucleus, area postrema (AP), nucleus tractus solitarius, and dorsal motor nucleus of the vagus. The PP receptor differs from neuropeptide Y and peptide YY receptors in its binding specificity and location. Because PP is not produced in the brain, and the blood-brain barrier (BBB) excludes circulating peptides from most areas in the brain, we employed an in vivo radioreceptor assay to determine whether circulating PP binds to areas such as the AP that has both an incomplete BBB and a high concentration of PP receptors. 125I-PP and 131I-bovine serum albumin were infused simultaneously into rats through a peripheral vein with or without excess unlabeled PP. After 10 min, rats were killed and the brains were removed and cut into eight regions based on the autoradiographic localization of PP receptors. There was a significant (P less than 0.02) increase in saturable radiolabeled PP accumulation in the region that included the AP, demonstrating that circulating PP can bind to this area of the brain in vivo. PP is released into the circulation after a meal via mechanisms that exhibit vagal and cholinergic dependence. We speculate that PP completes a feedback loop by binding to receptors in the AP and interacting with the adjacent vagal nuclei to inhibit vagal activity.

摘要

胰多肽(PP)通过可能由中枢介导的间接机制抑制胰腺外分泌。导致胰腺分泌受抑制的PP的中枢作用位点尚未确定。利用放射自显影技术鉴定大鼠脑冰冻切片上的125I-PP结合情况,我们在缰核、最后区(AP)、孤束核和迷走神经背运动核中发现了高浓度的可饱和、高亲和力PP受体。PP受体在结合特异性和位置上与神经肽Y和肽YY受体不同。由于脑中不产生PP,且血脑屏障(BBB)将循环肽排除在脑的大多数区域之外,我们采用体内放射受体分析法来确定循环中的PP是否与既有不完整血脑屏障又有高浓度PP受体的区域(如AP)结合。将125I-PP和131I-牛血清白蛋白通过外周静脉同时注入大鼠体内,有或没有过量未标记的PP。10分钟后,处死大鼠,取出大脑并根据PP受体的放射自显影定位切成八个区域。在包括AP的区域中,可饱和放射性标记的PP积累有显著增加(P小于0.02),表明循环中的PP在体内可与脑的该区域结合。进食后,PP通过表现出迷走神经和胆碱能依赖性的机制释放到循环中。我们推测,PP通过与AP中的受体结合并与相邻的迷走神经核相互作用以抑制迷走神经活动,从而完成一个反馈回路。

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