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猪血管活性肠肽与豚鼠分散胰腺腺泡细胞的相互作用。血管活性肠肽和促胰液素对细胞3':5'-单磷酸腺苷作用的结构要求。

Interaction of porcine vasoactive intestinal peptide with dispersed pancreatic acinar cells from the guinea pig. Structural requirements for effects of vasoactive intestinal peptide and secretin on cellular adenosine 3':5'-monophosphate.

作者信息

Robberecht P, Conlon T P, Gardner J D

出版信息

J Biol Chem. 1976 Aug 10;251(15):4635-9.

PMID:181379
Abstract

Secretin and vasoactive intestinal peptide (VIP), but not glucagon, stimulate accumulation of cyclic AMP in dispersed guinea pig pancreatic acinar cells. Secretin stimulated cellular accumulation of cyclic AMP by interacting with a single class of high affinity receptors. On the other hand, the dose-response curve for VIP-stimulated cellular cyclic AMP was biphasic and reflected interaction of this peptide with two classes of receptors. Results obtained with synthetic fragments of VIP and secretin indicate that the receptor having a high affinity for VIP has a low affinity for secretin, interacts with, but does not distinguish among, secretin, secretin 5-27 and [6-tyrosine] secretin or among secretin 14-27, VIP 14-28, VIP 15-28, and increases cellular cyclic AMP when occupied by VIP, but not when occupied by secretin, [6-tyrosine] secretin, or secretin 1-14. The receptor having a low affinity for VIP has a high affinity for secretin, interacts with and distinguishes among secretin, secretin 5-27, and [6-tyrosine] secretin, interacts with secretin 14-27 but not with VIP 14-28 or VIP 15-28, and increases cellular cyclic AMP when occupied by VIP, secretin, [6-tyrosine] secretin, or secretin 1-14.

摘要

促胰液素和血管活性肠肽(VIP)可刺激豚鼠胰腺分散腺泡细胞中环状AMP的积累,而胰高血糖素则无此作用。促胰液素通过与一类高亲和力受体相互作用来刺激细胞中环状AMP的积累。另一方面,VIP刺激细胞环状AMP的剂量反应曲线呈双相性,反映了该肽与两类受体的相互作用。用VIP和促胰液素的合成片段所获得的结果表明,对VIP具有高亲和力的受体对促胰液素具有低亲和力,它可与促胰液素、促胰液素5 - 27和[6 - 酪氨酸]促胰液素相互作用,但不能区分它们,也不能区分促胰液素14 - 27、VIP 14 - 28、VIP 15 - 28;当被VIP占据时可增加细胞环状AMP,但被促胰液素、[6 - 酪氨酸]促胰液素或促胰液素1 - 14占据时则不能增加。对VIP具有低亲和力的受体对促胰液素具有高亲和力,它可与促胰液素、促胰液素5 - 27和[6 - 酪氨酸]促胰液素相互作用并能区分它们,可与促胰液素14 - 27相互作用,但不与VIP 14 - 28或VIP 15 - 28相互作用;当被VIP、促胰液素、[6 - 酪氨酸]促胰液素或促胰液素1 - 14占据时可增加细胞环状AMP。

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