首页> 外文期刊>Cell Calcium: The International Interdisciplinary Forum for Research on Calcium >Vasoactive intestinal peptide (VIP) stimulates (Ca(2+))(i)and cyclic AMPin CHO cells expressing Galpha16.
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Vasoactive intestinal peptide (VIP) stimulates (Ca(2+))(i)and cyclic AMPin CHO cells expressing Galpha16.

机译:血管活性肠肽(VIP)刺激(Ca(2 +))(i)和表达Galpha16的环状AMPin CHO细胞。

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摘要

The stimulatory effect of vasoactive intestinal peptide (VIP) and analogues on [Ca(2+)](i)has been investigated in chinese hamster ovary (CHO) cells stably transfected with the reporter gene aequorin, and expressing either the human VPAC(1)or VPAC(2)receptor in absence or in presence of the Galpha16. In cells that were not transfected with Galpha16 and expressed a similar density of receptors, the VIP induced [Ca(2+)](i)increase was higher in VPAC(1)than in VPAC(2)receptor expressing cells. In aequorin/Galpha16 cotransfected cells, the VIP-induced response was higher, reaching 70 to 80% of the maximal calcium response, obtained after digitonin treatment, in response to both VPAC(1)and VPAC(2)receptor stimulation.The results suggest that in hematopoietic cells, which express both VIP receptors and Galpha16, the signalling pathway of VIP could be mediated through both cyclic AMP and [Ca(2+)](i)increase.
机译:已经在稳定转染报告基因水母发光蛋白并表达人VPAC(1)的中国仓鼠卵巢(CHO)细胞中研究了血管活性肠肽(VIP)和类似物对[Ca(2 +)](i)的刺激作用。或没有Galpha16的VPAC(2)受体。在未转染Galpha16并表达相似密度受体的细胞中,VPAC诱导的[Ca(2 +)](i)升高在VPAC(1)中高于在VPAC(2)受体表达细胞中。在水母发光蛋白/ Galpha16共转染的细胞中,VIP诱导的响应较高,达到了洋地黄素处理后对VPAC(1)和VPAC(2)受体刺激的最大钙响应的70%至80%。在同时表达VIP受体和Galpha16的造血细胞中,VIP的信号通路可以通过环AMP和[Ca(2 +)](i)的增加来介导。

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