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从人血中分离出一种新型内源性阿片类镇痛药。

Isolation of a novel endogenous opiate analgesic from human blood.

作者信息

Pert C B, Pert A, Tallman J F

出版信息

Proc Natl Acad Sci U S A. 1976 Jul;73(7):2226-30. doi: 10.1073/pnas.73.7.2226.

Abstract

Based upon its ability to inhibit opiate receptor binding, a low-molecular-weight substance (600) has been isolated from human plasma by extraction into butanol and ion exchange, molecular sieve, and thin-layer chromatography. When this substance, termed anodynin, is microinjected into rat periaqueductal gray matter, it causes a profound, long-lasting analgesia which is prevented by prior injection of the opiate antagonist naloxone. Anodynin (opiate receptor binding material) levels in serum from hypophysectomized rats are less than 5% of values obtained in sham-operated controls. Anodynin differs from enkephalin, a morphine-like peptide isolated from brain, in its sensitivity to enzymatic loss of opiate receptor inhibitory potency, thin-layer chromatographic mobility, and behavioral effects. Anodynin might be a hormone that acts on peripheral opiate receptors in the classical manner, but might also, due to its lipophilic nature and small size, penetrate into the brain to produce centrally mediated behavioral effects.

摘要

基于其抑制阿片受体结合的能力,通过丁醇萃取、离子交换、分子筛和薄层色谱法,从人血浆中分离出一种低分子量物质(600)。当将这种称为止痛素的物质微量注射到大鼠导水管周围灰质中时,会引起深度、持久的镇痛作用,而预先注射阿片拮抗剂纳洛酮可阻止这种作用。垂体切除大鼠血清中的止痛素(阿片受体结合物质)水平不到假手术对照组的5%。止痛素与从脑中分离出的一种吗啡样肽脑啡肽不同,在对阿片受体抑制效力的酶促丧失、薄层色谱迁移率和行为效应的敏感性方面存在差异。止痛素可能是一种以经典方式作用于外周阿片受体的激素,但由于其亲脂性和小尺寸,也可能穿透进入大脑产生中枢介导的行为效应。

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