前列腺素可抑制从离体大鼠胃肠嗜铬样细胞分泌组胺和胰抑制素。

Prostaglandins inhibit secretion of histamine and pancreastatin from isolated rat stomach ECL cells.

作者信息

Lindström E, Håkanson R

机构信息

Department of Pharmacology, University of Lund, Sweden.

出版信息

Br J Pharmacol. 1998 Jul;124(6):1307-13. doi: 10.1038/sj.bjp.0701953.

DOI:10.1038/sj.bjp.0701953

PMID:9720805

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565508/

Abstract

The present study examines the effect of naturally occurring prostanoids and prostaglandin (PG) congeners on gastrin- and pituitary adenylate cyclase-activating peptide (PACAP)-evoked histamine and pancreastatin secretion from isolated rat stomach ECL cells. 2. ECL cells (75-85% purity) were isolated from rat stomach using pronase digestion followed by repeated counter-flow elutriation and cultured for 48 h before secretion experiments. The release of histamine and pancreastatin was determined by radioimmunoassay. 3. None of the PGs tested stimulated the release of either histamine or pancreastatin. 4. PGE1 and PGE2 inhibited both gastrin- and PACAP-evoked histamine and pancreastatin secretion (IC50 = 1-2 x 10(-10) M). Most other naturally occuring prostanoids and PG congeners had no or little inhibitory effect. The PGE analogues misoprostol and sulprostone were more potent (IC50 = 0.9 x 10(-11) M and 2 x 10(-11) M respectively) than PGE1 and PGE2. The rank order of potency was misoprostol > sulprostone > PGE1 = PGE2, suggesting the involvement of the so-called EP3 receptor. 5. The effects of PGs on the stomach ECL cells may be direct or indirect, for instance through the stimulated release of somatostatin from contaminating D cells (2-3%). However, the amount of somatostatin in the cell culture after 48 h was below the limit of detection, and somatostatin immunoneutralization did not prevent misoprostol from inhibiting secretion from the ECL cells. 6. The misoprostol-induced inhibition was reversed by pertussis toxin suggesting the involvement of G-protein subunits G alpha(0) and/or G alpha(i). 7. In view of the potency by which PGE1, PGE2, misoprostol and sulprostone inhibited the stimulated release of histamine and pancreastatin, we suggest that the ECL cells represent a primary target for prostaglandins acting via an EP3 receptor in the oxyntic mucosa. 8. The results suggest that the clinically useful effect of misoprostol as an anti-ulcer drug reflects its ability to inhibit stomach ECL-cell histamine secretion.

摘要

本研究考察了天然存在的前列腺素及其类似物对胃泌素和垂体腺苷酸环化酶激活肽（PACAP）诱发的大鼠离体胃肠嗜铬样（ECL）细胞组胺和胰抑制素分泌的影响。2. 采用链霉蛋白酶消化，随后反复逆流淘析从大鼠胃中分离出纯度为75 - 85%的ECL细胞，并在分泌实验前培养48小时。组胺和胰抑制素的释放通过放射免疫测定法测定。3. 所测试的前列腺素均未刺激组胺或胰抑制素的释放。4. PGE1和PGE2抑制胃泌素和PACAP诱发的组胺和胰抑制素分泌（IC50 = 1 - 2×10⁻¹⁰ M）。大多数其他天然存在的前列腺素及其类似物没有或只有轻微的抑制作用。PGE类似物米索前列醇和舒前列素比PGE1和PGE2更有效（IC50分别为0.9×10⁻¹¹ M和2×10⁻¹¹ M）。效力顺序为米索前列醇＞舒前列素＞PGE1 = PGE2，提示所谓的EP3受体参与其中。5. 前列腺素对胃ECL细胞的作用可能是直接的或间接的，例如通过刺激污染的D细胞（2 - 3%）释放生长抑素。然而，48小时后细胞培养物中生长抑素的量低于检测限，并且生长抑素免疫中和并不能阻止米索前列醇抑制ECL细胞的分泌。6. 百日咳毒素可逆转米索前列醇诱导的抑制作用，提示G蛋白亚基Gα(0)和/或Gα(i)参与其中。7. 鉴于PGE1、PGE2、米索前列醇和舒前列素抑制组胺和胰抑制素刺激释放的效力，我们认为ECL细胞是前列腺素通过胃黏膜中的EP3受体发挥作用的主要靶点。8. 结果表明，米索前列醇作为抗溃疡药物的临床有效作用反映了其抑制胃ECL细胞组胺分泌的能力。