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速激肽和神经激肽A是NK-1受体上的高亲和力配体:来自同源与异源结合分析的证据。

Septide and neurokinin A are high-affinity ligands on the NK-1 receptor: evidence from homologous versus heterologous binding analysis.

作者信息

Hastrup H, Schwartz T W

机构信息

Laboratory for Molecular Pharmacology, Rigshospitalet 6321, Copenhagen, Denmark.

出版信息

FEBS Lett. 1996 Dec 16;399(3):264-6. doi: 10.1016/s0014-5793(96)01337-3.

Abstract

The three main tachykinins, substance P, neurokinin A (NKA), and neurokinin B, are believed to be selective ligands for respectively the NK-1, NK-2 and NK-3 receptors. However, NKA also has actions which cannot be mediated through its normal NK-2 receptor and the synthetic peptide [pGlu6,Pro9]-Substance P9-11--called septide--is known to have tachykinin-like actions despite its apparent lack of binding to any known tachykinin receptor. In the cloned NK-1 receptor expressed in COS-7 cells NKA and septide as expected were poor competitors for radiolabeled substance P. However, by using radiolabeled NKA and septide directly, it was found that both peptides in homologous binding assays as well as in competition against each other in fact bound to the NK-1 receptor with high affinity: Kd values of 0.51 +/- 0.15 nM (NKA) and 0.55 +/- 0.03 nM (septide). It is concluded that NKA and septide are high-affinity ligands for the NK-1 receptor but that they are poor competitors for substance P, which in contrast competes very well for binding with both NKA and septide.

摘要

三种主要的速激肽,即P物质、神经激肽A(NKA)和神经激肽B,被认为分别是NK-1、NK-2和NK-3受体的选择性配体。然而,NKA也具有一些无法通过其正常的NK-2受体介导的作用,并且合成肽[pGlu6,Pro9]-P物质9-11(称为七肽)尽管明显不与任何已知的速激肽受体结合,但已知具有速激肽样作用。在COS-7细胞中表达的克隆NK-1受体中,正如预期的那样,NKA和七肽对放射性标记的P物质是较弱的竞争剂。然而,通过直接使用放射性标记的NKA和七肽,发现在同源结合试验中以及在相互竞争中,这两种肽实际上都以高亲和力与NK-1受体结合:NKA的解离常数(Kd)值为0.51±0.15 nM,七肽的Kd值为0.55±0.03 nM。结论是,NKA和七肽是NK-1受体的高亲和力配体,但它们对P物质是较弱的竞争剂,相反,P物质与NKA和七肽的结合竞争非常有效。

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