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环磷酸鸟苷在器官培养的大鼠胃窦黏膜胃泌素分泌中的作用。

Role of cyclic GMP in gastrin secretion from rat antral mucosae in organ culture.

作者信息

Lamprecht S A, Schwartz B, Krugliak P, Odes H S, Guberman R, Krawiec J

出版信息

J Cyclic Nucleotide Protein Phosphor Res. 1986;11(3):177-89.

PMID:2876015
Abstract

Rat antral mucosae maintained for 6 h in organ culture responded to carbamylcholine with a significant increase in endogenous cyclic GMP production and gastrin secretion. The acetylcholine analogue exerted a stimulatory action within a defined concentration range: exposure of antral explants to carbachol concentrations greater than the optimal stimulatory dose was accompanied by a marked decrease in both cyclic GMP production and gastrin release. Exogenous 8-Br-cyclic GMP (1 mM) significantly augmented gastrin secretion into the culture media during 6-12 h culture periods. Cycloheximide (0.1 mM) and the Ca2+ channel-blocker verapamil (5 microM) prevented 8-Br-cyclic GMP from acting as a gastrin secretagogue. Addition of cyclic somatostatin-14 (0.1 mM) to culture media was attended by complete inhibition of 8-Br-cyclic GMP-stimulable gastrin secretion. These results provide evidence that cyclic GMP may play a mediatory role in the coupling of gastrin secretory processes to agonist stimulation. It would seem that the secretagogue action of 8-Br-cyclic GMP requires unabated Ca2+ transmembrane fluxes and protein biosynthesis. Since somatostatin-14 abrogates the stimulatory effect of 8-Br-cyclic GMP on antral gastrin secretion, it is surmised that the inhibitory tetradecapeptide acts at a locus (or loci) distal to domains involved in the actual generation of the cyclic nucleotide.

摘要

在器官培养中维持6小时的大鼠胃窦黏膜对氨甲酰胆碱有反应,内源性环鸟苷酸(cGMP)生成和胃泌素分泌显著增加。乙酰胆碱类似物在一定浓度范围内发挥刺激作用:胃窦外植体暴露于大于最佳刺激剂量的卡巴胆碱浓度时,cGMP生成和胃泌素释放均显著降低。在6 - 12小时的培养期间,外源性8 - 溴环鸟苷酸(1 mM)显著增加了胃泌素向培养基中的分泌。环己酰亚胺(0.1 mM)和钙通道阻滞剂维拉帕米(5 microM)阻止了8 - 溴环鸟苷酸作为胃泌素促分泌剂发挥作用。向培养基中添加环生长抑素 - 14(0.1 mM)会完全抑制8 - 溴环鸟苷酸刺激的胃泌素分泌。这些结果提供了证据,表明环鸟苷酸可能在胃泌素分泌过程与激动剂刺激的偶联中起介导作用。似乎8 - 溴环鸟苷酸的促分泌作用需要持续的钙跨膜通量和蛋白质生物合成。由于生长抑素 - 14消除了8 - 溴环鸟苷酸对胃窦胃泌素分泌的刺激作用,推测这种抑制性十四肽作用于参与环核苷酸实际生成的结构域的远端位点(或多个位点)。

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