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壁细胞中钙离子依赖性和环磷酸腺苷依赖性刺激途径之间的相互作用。

Interactions between Ca2+- and cAMP-dependent stimulatory pathways in parietal cells.

作者信息

Li Z Q, Mårdh S

机构信息

Department of Cell Biology, Faculty of Health Sciences Linköping University, Sweden.

出版信息

Biochim Biophys Acta. 1996 Apr 24;1311(2):133-42. doi: 10.1016/0167-4889(96)00006-7.

Abstract

Isolated rat parietal cells were used to investigate the role of intracellular Ca2+ in the action of cAMP-dependent secretagogues and cross talk between cAMP- and Ca2+ -dependent stimulatory pathways. Aminopyrine accumulation (an index of acid produced and trapped by the parietal cells), cytosolic free Ca2+, morphological transformation and cell viability were used to investigate parietal cell function and stimulation. The increase of cytosolic free Ca2+ promoted by gastrin, or carbachol, was abolished by the intracellular Ca2+ chelator 1,2-bis(2-aminophenoxy)ethane-N,N,N',N'-tetraacetic acid (BAPTA, 10 microM). Also, the morphological transformations induced by dibutyryladenosine 3':5'-cyclic monophosphate (DBcAMP), gastrin, and Sp-adenosine-cyclic-3', 5'-monophosphothioate (Sp-cAMPS) were completely abolished by BAPTA (10 microM). In aminopyrine accumulation the action of 1 mM DBcAMP was dose-dependently reduced by BAPTA. The Ca2+ ionophore A23187 alone, in the range of 1 pM to 1 microM, had no effect but it dose-dependently potentiated the action of 1 mM DBcAMP in aminopyrine accumulation. The inhibitory actions of BAPTA on DBcAMP- and histamine-stimulated aminopyrine accumulation were dose-dependently reversed by A23187. Histamine-stimulated protein kinase activity and viability parameters as cellular lactate dehydrogenase (LDH) and trypan blue exclusion were not changed by BAPTA. These results indicated that in isolated parietal cells: (1) the action of cAMP-dependent secretagogues in aminopyrine accumulation and morphological transformation are dependent on cytosolic free Ca2+; (2) Ca2+ -induced morphological transformation is essential for aminopyrine accumulation; (3) a threshold level of one second messenger is required for stimulation of aminopyrine accumulation by the other second messenger.

摘要

分离的大鼠壁细胞用于研究细胞内Ca2+在环磷酸腺苷(cAMP)依赖性促分泌剂作用中的作用以及cAMP和Ca2+依赖性刺激途径之间的相互作用。氨基比林蓄积(壁细胞产生并捕获的酸的指标)、胞质游离Ca2+、形态转化和细胞活力用于研究壁细胞功能和刺激情况。胃泌素或卡巴胆碱促进的胞质游离Ca2+增加被细胞内Ca2+螯合剂1,2-双(2-氨基苯氧基)乙烷-N,N,N',N'-四乙酸(BAPTA,10微摩尔)消除。此外,二丁酰腺苷3':5'-环一磷酸(DBcAMP)、胃泌素和Sp-腺苷-环-3',5'-单磷酸硫代物(Sp-cAMPS)诱导的形态转化被BAPTA(10微摩尔)完全消除。在氨基比林蓄积方面,1毫摩尔DBcAMP的作用被BAPTA剂量依赖性降低。单独的Ca2+离子载体A23187在1皮摩尔至1微摩尔范围内无作用,但它在氨基比林蓄积中剂量依赖性增强1毫摩尔DBcAMP的作用。BAPTA对DBcAMP和组胺刺激的氨基比林蓄积的抑制作用被A23187剂量依赖性逆转。组胺刺激的蛋白激酶活性以及作为细胞乳酸脱氢酶(LDH)和台盼蓝排斥率的活力参数不受BAPTA影响。这些结果表明,在分离的壁细胞中:(1)cAMP依赖性促分泌剂在氨基比林蓄积和形态转化中的作用依赖于胞质游离Ca2+;(2)Ca2+诱导的形态转化对于氨基比林蓄积至关重要;(3)一种第二信使刺激氨基比林蓄积需要另一种第二信使达到阈值水平。

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