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胃泌素对分离的猪壁细胞中氨基比林蓄积的作用需要环磷酸腺苷(cAMP)。

Gastrin action on aminopyrine accumulation in isolated pig parietal cells requires cAMP.

作者信息

Cabero J L, Li Z Q, Mårdh S

机构信息

Department of Medical and Physiological Chemistry, Uppsala University, Sweden.

出版信息

Biochim Biophys Acta. 1993 Jun 30;1177(3):245-52. doi: 10.1016/0167-4889(93)90120-e.

Abstract

The mechanism of action of gastrin on pig parietal cells was investigated. The aminopyrine accumulation technique was used to estimate acid production in gastric mucosal cells, containing 10-20% parietal cells, and in enriched parietal cells, containing 65-95% parietal cells. The gastrin analogue pentagastrin stimulated aminopyrine accumulation in a dose-dependent fashion irrespective of the proportion of non-parietal cells present. The apparent EC50 for pentagastrin was 5 nM and the maximally effective concentration was 100 nM. The histamine H2-receptor antagonist ranitidine did not affect the action of pentagastrin. The stimulatory effects of various doses of histamine on aminopyrine accumulation in highly enriched parietal cells were potentiated by the inclusion of 100 nM pentagastrin in the incubation medium. In another series of experiments using mucosal cells, the action of effective doses of pentagastrin were potentiated by the phosphodiesterase inhibitor isobutylmethyl xanthine (IBMX), which alone elicited an aminopyrine accumulation equal to 50% of that obtained by 100 microM histamine. When ranitidine (100 microM) was included, the action of IBMX was almost completely abolished. However, the dose-response curve for pentagastrin in the presence of ranitidine plus IBMX was similar to that obtained in the absence of IBMX. Dibutyryl-cAMP (DBcAMP, 1 mM) in the presence of ranitidine (100 microM) also potentiated the action of all effective doses of pentagastrin on mucosal cells. The protein kinase A inhibitor Rp-cAMPS, present at 500 microM in the incubation medium, significantly reduced the action of each effective concentration of pentagastrin on aminopyrine accumulation in enriched parietal cells. These results in pig parietal cells were interpreted as indicative of: (i) an action of gastrin exerted directly on the parietal cells; (ii) elevation of intracellular cAMP having a permissive role in the action of gastrin on aminopyrine accumulation.

摘要

研究了胃泌素对猪壁细胞的作用机制。采用氨基比林蓄积技术来评估含10 - 20%壁细胞的胃黏膜细胞以及含65 - 95%壁细胞的富集壁细胞中的酸分泌。胃泌素类似物五肽胃泌素以剂量依赖方式刺激氨基比林蓄积,与非壁细胞的比例无关。五肽胃泌素的表观EC50为5 nM,最大有效浓度为100 nM。组胺H2受体拮抗剂雷尼替丁不影响五肽胃泌素的作用。在孵育培养基中加入100 nM五肽胃泌素可增强不同剂量组胺对高度富集壁细胞中氨基比林蓄积的刺激作用。在另一系列使用黏膜细胞的实验中,磷酸二酯酶抑制剂异丁基甲基黄嘌呤(IBMX)增强了有效剂量五肽胃泌素的作用,单独使用时IBMX引起的氨基比林蓄积相当于100 μM组胺所引起蓄积的50%。当加入雷尼替丁(100 μM)时,IBMX的作用几乎完全被消除。然而,在雷尼替丁加IBMX存在时五肽胃泌素的剂量 - 反应曲线与未加IBMX时相似。在雷尼替丁(100 μM)存在下,二丁酰 - cAMP(DBcAMP,1 mM)也增强了所有有效剂量五肽胃泌素对黏膜细胞的作用。孵育培养基中存在的500 μM蛋白激酶A抑制剂Rp - cAMPS显著降低了各有效浓度五肽胃泌素对富集壁细胞中氨基比林蓄积的作用。猪壁细胞的这些结果被解释为表明:(i)胃泌素直接作用于壁细胞;(ii)细胞内cAMP升高在胃泌素对氨基比林蓄积的作用中起允许作用。

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