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从酪蛋白胰蛋白酶水解产物中获得的两种缓激肽增强肽的生化和药理学特性

Biochemical and pharmacological aspects of two bradykinin-potentiating peptides obtained from tryptic hydrolysis of casein.

作者信息

Perpetuo Elen A, Juliano Luis, Lebrun Ivo

机构信息

Laboratory of Biochemistry and Biophysics, Butantan Institute, Av Vital Brazil 1500, São Paulo, SP, 05503-900, Brazil.

出版信息

J Protein Chem. 2003 Nov;22(7-8):601-6. doi: 10.1023/b:jopc.0000008724.98339.ff.

DOI:10.1023/b:jopc.0000008724.98339.ff
PMID:14714726
Abstract

Peptides that display bradykinin-potentiating activity have been obtained from a number of distinct sources, such as snake venoms, fibrinogen, and casein. This paper describes the characterization of two new peptides generated by tryptic hydrolysis of casein. No homology was found with other known vasoactive or vasopotentiating peptides, especially by the lack of Ile-Pro-Pro motif. The peptides EMPFPK and YPVEPFTE, corresponding to the gamma casein sequence (108-113 and 114-121, respectively), displayed a selective potentiating activity on isolated guinea pig ileum for bradykinin. Besides, the octapeptide YPVEPFTE showed an in vitro competitive inhibitor effect on angiotensin-converting enzyme and thimet oligopeptidase and presented an opiate-like activity, increasing two times the latence time in the hot-plate assay. The results suggest that the isolated bioactive peptides act on conversion and/or inactivation of endogenous peptides by enzymes such as angiotensin-converting enzyme and thimet oligopeptidase by modifying several systemic responses such as blood-pressure regulation and in pain response.

摘要

具有缓激肽增强活性的肽已从多种不同来源获得,如蛇毒、纤维蛋白原和酪蛋白。本文描述了通过胰蛋白酶水解酪蛋白产生的两种新肽的特性。未发现与其他已知的血管活性或血管增强肽有同源性,尤其是缺乏异亮氨酸 - 脯氨酸 - 脯氨酸基序。对应于γ-酪蛋白序列(分别为108 - 113和114 - 121)的肽EMPFPK和YPVEPFTE对分离的豚鼠回肠中的缓激肽表现出选择性增强活性。此外,八肽YPVEPFTE对血管紧张素转换酶和硫醚氨酸寡肽酶表现出体外竞争性抑制作用,并呈现出阿片样活性,在热板试验中使潜伏期增加两倍。结果表明,分离出的生物活性肽通过修饰多种全身反应,如血压调节和疼痛反应,作用于血管紧张素转换酶和硫醚氨酸寡肽酶等酶对内源性肽的转化和/或失活。

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