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人神经激肽-3受体的cDNA序列及异源表达

cDNA sequence and heterologous expression of the human neurokinin-3 receptor.

作者信息

Huang R R, Cheung A H, Mazina K E, Strader C D, Fong T M

机构信息

Department of Molecular Pharmacology and Biochemistry, Merck Research Laboratories, Rahway, NJ 07065.

出版信息

Biochem Biophys Res Commun. 1992 Apr 30;184(2):966-72. doi: 10.1016/0006-291x(92)90685-e.

Abstract

Functional cDNA clones encoding the human neurokinin-3 receptor were isolated from human brain mRNA. The cloned human neurokinin-3 receptor was expressed in COS cells and Xenopus oocytes, where peptide binding affinity and intracellular effector activation were determined. Neurokinin B is the most potent agonist, followed by eledoisin, substance K and substance P. The binding affinities of these peptides at the human neurokinin-3 receptor differ quantitatively from the rat receptor, implying a functional consequence of the sequence divergence between the two species. Heterologous expression in oocytes revealed that, unlike the neurokinin-1 receptor, the efficacy of ion channel activation mediated by the neurokinin-3 receptor does not approximate the binding affinity. The heterologous expression of the human neurokinin-3 receptor will facilitate further investigation into its biochemical functions.

摘要

从人脑海马体mRNA中分离出编码人神经激肽-3受体的功能性cDNA克隆。克隆出的人神经激肽-3受体在COS细胞和非洲爪蟾卵母细胞中表达,测定了其肽结合亲和力和细胞内效应器激活情况。神经激肽B是最有效的激动剂,其次是蛙皮素、神经激肽K和P物质。这些肽在人神经激肽-3受体上的结合亲和力与大鼠受体在数量上有所不同,这意味着两个物种之间序列差异的功能后果。在卵母细胞中的异源表达表明,与神经激肽-1受体不同,神经激肽-3受体介导的离子通道激活效率与结合亲和力并不接近。人神经激肽-3受体的异源表达将有助于进一步研究其生化功能。

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