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APJ的分子与功能特性。mRNA的组织分布及其与内源性配体apelin的相互作用。

Molecular and functional characteristics of APJ. Tissue distribution of mRNA and interaction with the endogenous ligand apelin.

作者信息

Hosoya M, Kawamata Y, Fukusumi S, Fujii R, Habata Y, Hinuma S, Kitada C, Honda S, Kurokawa T, Onda H, Nishimura O, Fujino M

机构信息

Discovery Research Division, Takeda Chemical Industries Ltd., Wadai 10, Tsukuba, Ibaraki 300-4293, Japan.

出版信息

J Biol Chem. 2000 Jul 14;275(28):21061-7. doi: 10.1074/jbc.M908417199.

Abstract

We have recently identified apelin as the endogenous ligand for human APJ. In rats, the highest expression of APJ mRNA was detected in the lung, suggesting that APJ and its ligand play an important role in the pulmonary system. When apelin-36 and its pyroglutamylated C-terminal peptide, [<Glu(65)]apelin-13, were compared in microphysiometric analyses, the elevation of extracellular acidification induced in cells expressing APJ by [<Glu(65)]apelin-13 was transient, whereas that by apelin-36 was sustained. These responses were almost completely inhibited by a specific inhibitor for G(i) or that for Na(+)/H(+) exchanger. (125)I -Labeled [<Glu(65)]apelin-13 analogue specifically bound to APJ with a high affinity, and [<Glu(65)]apelin-13 was more potent than apelin-36 in competitive inhibition assays. Because pretreatment with apelin-36 but not [<Glu(65)]apelin-13 drastically reduced the binding of the labeled apelin to APJ, the different patterns of acidification induced by these two peptides appeared to reflect their dissociation rather than association with APJ. Apelin elicited the migration of APJ-expressing cells, and [<Glu(65)]apelin-13 was more potent than apelin-36 in this activity. Heterogeneous molecular forms of apelin corresponding to apelin-36 and [<Glu(65)]apelin-13 were produced in bovine colostrum. Apelin-36 and [<Glu(65)]apelin-13 might have different functions in vivo and in vitro.

摘要

我们最近鉴定出apelin是人类APJ的内源性配体。在大鼠中,肺中检测到APJ mRNA的最高表达,这表明APJ及其配体在肺系统中发挥重要作用。在微生理分析中比较apelin-36及其焦谷氨酸化的C末端肽[<Glu(65)]apelin-13时,[<Glu(65)]apelin-13诱导表达APJ的细胞中细胞外酸化的升高是短暂的,而apelin-36诱导的则是持续的。这些反应几乎完全被G(i)特异性抑制剂或Na(+)/H(+)交换体特异性抑制剂抑制。(125)I标记的[<Glu(65)]apelin-13类似物以高亲和力特异性结合APJ,并且在竞争抑制试验中[<Glu(65)]apelin-13比apelin-36更有效。因为用apelin-36预处理而非[<Glu(65)]apelin-13预处理可显著降低标记的apelin与APJ的结合,所以这两种肽诱导的不同酸化模式似乎反映了它们与APJ的解离而非结合。Apelin引起表达APJ的细胞迁移,并且在该活性中[<Glu(65)]apelin-13比apelin-36更有效。在牛初乳中产生了与apelin-36和[<Glu(65)]apelin-13相对应的apelin异质分子形式。Apelin-36和[<Glu(65)]apelin-13在体内和体外可能具有不同的功能。

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