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首页> 外文期刊>Peptides: An International Journal >Interaction of xenin with the neurotensin receptor of guinea pig enteral smooth muscles.
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Interaction of xenin with the neurotensin receptor of guinea pig enteral smooth muscles.

机译:Xenin与豚鼠肠内平滑肌神经降压素受体的相互作用。

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摘要

Xenin, a 25 aminoacid peptide, interacts with the neurotensin receptor subtype 1 of intestinal muscles of the guinea pig. Replacement of the C-terminal Lys -Arg peptide bond in xenin 6 by a reduced pseudo-peptide bond augmented binding affinity to isolated jejunal and colonic muscle membranes by factors of 7.7 and 21.0 respectively; the potency to contract the jejunum and to relax the colon was increased by factors of 3.2 and 1.3. The C-terminus Trp-Ile-Leu (WIL) of xenin, in contrast to the C-terminus Tyr-Ile-Leu (YIL) of neurotensin, bound competitively to the muscle membranes. WIL blocked the contractile action of xenin in the jejunum and was synergistic with the relaxing action in the colon. The Lys -Arg motif and Trp in the C-terminus of xenin are essential structures in the action of xenin on the enteral smooth muscle receptors.
机译:Xenin是一种25个氨基酸的肽,它与豚鼠肠道肌肉的神经降压素受体亚型1相互作用。用减少的伪肽键代替Xenin 6中C端Lys -Arg肽键,使与分离的空肠和结肠肌膜的结合亲和力分别增加7.7和21.0倍;空肠收缩和放松结肠的能力分别提高了3.2和1.3倍。与神经降压素的C末端Tyr-Ile-Leu(YIL)相比,Xenin的C末端Trp-Ile-Leu(WIL)与肌肉膜竞争性结合。 WIL阻止了Xenin在空肠中的收缩作用,并且与结肠中的松弛作用具有协同作用。 Xenin C末端的Lys -Arg基序和Trp是Xenin对肠平滑肌受体的作用中必不可少的结构。

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