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β-内啡肽:非哺乳动物同源物的镇痛及受体结合活性

beta-Endorphin: analgesic and receptor binding activity of non-mammalian homologs.

作者信息

Hammonds R G, Nicolas P, Li C H

出版信息

Int J Pept Protein Res. 1982 May;19(5):556-61. doi: 10.1111/j.1399-3011.1982.tb02642.x.

Abstract

Analgesic potencies of turkey, ostrich and des-acetyl salmon beta-endorphins have been measured in the tail-flick test and binding affinities determined by radio-receptor assay. The duration of analgesia and the slope of the dose-response curves generated by these peptides are similar to those elicited by mammalian beta-endorphins. This suggests that they act in vivo and in vitro on the same population of opiate receptors. The ratio of binding to analgesic potencies observed for these peptides varies nearly sixfold. Structure-activity analysis suggests that a basic side-chain at position 9 is required in order to produce a high opiate activity both in vivo and in vitro. A reexamination of the biological activities of camel beta-endorphin shows that the analgesic potency and binding affinity of this peptide are respectively 171 and 2.7 times higher than human beta-endorphin. His-27 and/or Gln-31 may contribute to this increased potency. The dissociation of radioreceptor binding affinity from analgesic potency in these naturally occurring beta-endorphin homologs suggests that either the conditions under which the binding assay is performed mask the true binding potency in the brain or that, once bound to the appropriate receptor, these homologs do not possess equal ability to produce biological effects.

摘要

已通过甩尾试验测定了火鸡、鸵鸟和去乙酰化鲑鱼β-内啡肽的镇痛效力,并通过放射受体分析法确定了它们的结合亲和力。这些肽产生的镇痛持续时间和剂量-反应曲线的斜率与哺乳动物β-内啡肽引起的相似。这表明它们在体内和体外作用于同一群阿片受体。观察到这些肽的结合与镇痛效力之比相差近六倍。结构-活性分析表明,为了在体内和体外产生高阿片活性,9位需要一个碱性侧链。对骆驼β-内啡肽生物活性的重新研究表明,该肽的镇痛效力和结合亲和力分别比人β-内啡肽高171倍和2.7倍。His-27和/或Gln-31可能促成了这种效力的增加。这些天然存在的β-内啡肽同系物中放射受体结合亲和力与镇痛效力的解离表明,要么进行结合测定的条件掩盖了大脑中的真实结合效力,要么一旦与适当的受体结合,这些同系物产生生物效应的能力并不相等。

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