胆囊收缩素对大鼠胰腺和胃生长的不同作用：胆囊收缩素（A）受体阻断的影响

Different actions of CCK on pancreatic and gastric growth in the rat: effect of CCK(A) receptor blockade.

作者信息

Varga G, Kisfalvi K, Pelosini I, D'Amato M, Scarpignato C

机构信息

Institute of Experimental Medicine, Hungarian Academy of Sciences, Budapest.

出版信息

Br J Pharmacol. 1998 Jun;124(3):435-40. doi: 10.1038/sj.bjp.0701811.

DOI:10.1038/sj.bjp.0701811

PMID:9647465

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565401/

Abstract

It is now well established that cholecystokinin (CCK) has a major physiological role in the regulation of pancreatic secretion and gastro-intestinal (GI) motility. Both these actions are mediated by stimulation of CCK(A)-receptors located on pancreatic acini and GI smooth muscle cells. While chronic administration of CCK-like peptides invariably causes pancreatic hypertrophy and hyperplasia, their action on gastric growth remains controversial. 2. In the present investigation the action of exogenous and endogenous CCK on both pancreatic and gastric growth was studied in the same animal. In addition, the ability of dexloxiglumide, a new potent and selective CCK(A)-receptor antagonist, to counteract CCK-mediated effects was evaluated. 3. The amphibian peptide caerulein (1 microg kg(-1) intraperitoneally three times daily) was used as a CCK agonist, while camostate (200 mg kg(-1) intragastrically once daily), a synthetic protease inhibitor, was used to release endogenous CCK. They were administered to rats for seven days with or without dexloxiglumide (25 mg kg(-1) subcutaneously 15 min before the stimulus). On the eighth day, animals were killed, the pancreas and stomach excised, weighed, homogenized and their protein and DNA content measured. 4. Both exogenous and endogenous CCK increased the weight of the pancreas as well as the total pancreatic protein and DNA content. Dexloxiglumide, which alone did not affect pancreatic size and composition, was able to counteract both caerulein- and camostate-induced pancreatic changes. Neither stimuli affected gastric growth in respect of weight and composition of the oxyntic gland area and the antrum. 5. These results show different effects of CCK on pancreatic and gastric growth. The CCK-induced pancreatic hypertrophy and hyperplasia are blocked by the potent and specific CCK(A)-receptor antagonist, dexloxiglumide. This compound therefore represents a useful tool to investigate CCK-receptor interactions in peripheral organs.

摘要

现已充分证实，胆囊收缩素（CCK）在调节胰腺分泌和胃肠（GI）蠕动方面具有重要的生理作用。这两种作用均由位于胰腺腺泡和胃肠平滑肌细胞上的CCK（A）受体的刺激介导。虽然长期给予CCK样肽总是会导致胰腺肥大和增生，但其对胃生长的作用仍存在争议。2. 在本研究中，在同一动物中研究了外源性和内源性CCK对胰腺和胃生长的作用。此外，评估了一种新型强效选择性CCK（A）受体拮抗剂右氯谷胺抵消CCK介导作用的能力。3. 两栖类肽蛙皮素（每天腹腔注射1μg kg⁻¹，共三次）用作CCK激动剂，而合成蛋白酶抑制剂卡莫司他（每天灌胃200mg kg⁻¹一次）用于释放内源性CCK。在有或没有右氯谷胺（刺激前15分钟皮下注射25mg kg⁻¹）的情况下，将它们给予大鼠七天。在第八天，处死动物，切除胰腺和胃，称重，匀浆并测量其蛋白质和DNA含量。4. 外源性和内源性CCK均增加了胰腺的重量以及胰腺总蛋白和DNA含量。单独使用时不影响胰腺大小和组成的右氯谷胺能够抵消蛙皮素和卡莫司他诱导的胰腺变化。两种刺激均未影响胃体腺区和胃窦的重量及组成方面的胃生长。5. 这些结果表明CCK对胰腺和胃生长有不同的作用。CCK诱导的胰腺肥大和增生被强效特异性CCK（A）受体拮抗剂右氯谷胺阻断。因此，该化合物是研究外周器官中CCK受体相互作用的有用工具。