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生长抑素受体亚型1、2和3对卡巴胆碱诱导的AR42J细胞中c-fos mRNA表达的调节

Regulation of carbachol-induced c-fos mRNA expression in AR42J cells by somatostatin receptor subtypes 1, 2, and 3.

作者信息

Cowles Robert A, Segura Bradley J, Mulholland Michael W

机构信息

Department of Surgery, University of Michigan Medical School, Ann Arbor, Michigan, USA.

出版信息

Pancreas. 2002 Oct;25(3):239-44. doi: 10.1097/00006676-200210000-00005.

DOI:10.1097/00006676-200210000-00005
PMID:12370534
Abstract

INTRODUCTION

Somatostatin is an inhibitory peptide that exerts its effects tissue-specifically by activating one or more of five receptors (SSTR 1-5). Although several studies have examined which SSTR subtypes control gastrointestinal function, effects of somatostatin on pancreatic gene expression are not well defined.

AIM

To examine the effects of somatostatin and newly synthesized selective SSTR agonists on the cholinergically stimulated expression of the immediate early response gene

METHODOLOGY AND RESULTS

In pancreatic acinar AR42J cells, polymerase chain reaction analysis revealed that mRNAs for SSTR 1, 2, and 3 were expressed. SSTR 4 and 5 were not detected. When AR42J cells were exposed to the cholinergic agonist carbachol in the presence of somatostatin or selective SSTR agonists, significant and dose-dependent reductions in agonist-induced levels of mRNA were noted. Pretreatment with agonists specific for SSTR 4 or 5 had no inhibitory effects. The inhibitory actions of somatostatin were pertussis toxin-sensitive. In addition, since somatostatin did not affect intracellular calcium homeostasis, the inhibitory actions of somatostatin are independent of calcium signaling.

CONCLUSION

The current studies demonstrate that somatostatin inhibits carbachol-induced increases in expression by interacting with somatostatin receptor subtypes 1, 2, and 3. In addition, because somatostatin did not affect intracellular calcium homeostasis, it can be concluded that SSTR actions are independent of carbachol-stimulated calcium signaling.

摘要

引言

生长抑素是一种抑制性肽,通过激活五种受体(SSTR 1 - 5)中的一种或多种来发挥其组织特异性作用。尽管有几项研究探讨了哪些SSTR亚型控制胃肠功能,但生长抑素对胰腺基因表达的影响尚不明确。

目的

研究生长抑素和新合成的选择性SSTR激动剂对胆碱能刺激的即刻早期反应基因表达的影响。

方法与结果

在胰腺腺泡AR42J细胞中,聚合酶链反应分析显示SSTR 1、2和3的mRNA有表达,未检测到SSTR 4和5。当AR42J细胞在生长抑素或选择性SSTR激动剂存在的情况下暴露于胆碱能激动剂卡巴胆碱时,观察到激动剂诱导的mRNA水平显著且呈剂量依赖性降低。用对SSTR 4或5特异的激动剂预处理没有抑制作用。生长抑素的抑制作用对百日咳毒素敏感。此外,由于生长抑素不影响细胞内钙稳态,所以生长抑素的抑制作用独立于钙信号传导。

结论

目前的研究表明,生长抑素通过与生长抑素受体亚型1、2和3相互作用来抑制卡巴胆碱诱导的表达增加。此外,由于生长抑素不影响细胞内钙稳态,可以得出结论,SSTR的作用独立于卡巴胆碱刺激的钙信号传导。

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