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新型缓激肽类似物对大鼠子宫收缩的影响

New bradykinin analogs in contraction of rat uterus.

作者信息

Trzeciak H I, Kozik W, Melhem S, Kania A, Dobrowolski D, Prahl A, Derdowska I, Lammek B

机构信息

Department of Pharmacology, Silesian Medical University, 40-752, Katowice, Poland.

出版信息

Peptides. 2000 Jun;21(6):829-34. doi: 10.1016/s0196-9781(00)00216-3.

Abstract

In this study, we evaluated 20 of our previously synthesized peptides on isolated rat uterus by Holton's procedure with minor modifications, and compared their activity with that assessed previously by their ability to inhibit vasodepressor response to exogenous bradykinin (BK) in conscious rats. We used [D-Arg(0), Hyp(3), Thi(5, 8), (D-Phe)(7)]BK, the B(2) antagonist of Vavrek and Stewart as a model when designing our analogs. We observed that, in the case of the rat uterus test, the activity of peptides modified by acylation of the N-terminus with various bulky groups depends substantially on the chemical character of the substituent. We also learned that, contrary to previous examples, acylation of the N-terminus of antagonists, which contain a sterically restricted fragment in the C-terminal part, may not improve their antagonistic potencies. Besides an improved characterization of a series BK analogs, our studies have provided new information on the structure-activity relationship, which in turn may be of value in the design of more potent and selective bradykinin antagonists. The results of our studies appear to support the hypothesis of others about the presence of different subtypes of B(2) receptors in rat uterus and blood vessels.

摘要

在本研究中,我们采用霍尔顿方法并略作修改,对20种我们之前合成的肽进行了离体大鼠子宫实验,并将它们的活性与之前通过抑制清醒大鼠对外源性缓激肽(BK)的血管降压反应能力所评估的活性进行比较。在设计类似物时,我们使用了Vavrek和Stewart的B₂拮抗剂[D-Arg(0), Hyp(3), Thi(5, 8), (D-Phe)(7)]BK作为模型。我们观察到,在大鼠子宫实验中,用各种庞大基团对N端进行酰化修饰的肽的活性很大程度上取决于取代基的化学性质。我们还了解到,与之前的例子相反,对于在C端含有空间位阻片段的拮抗剂,其N端的酰化修饰可能不会提高它们的拮抗效力。除了对一系列BK类似物有了更好的表征外,我们的研究还提供了有关构效关系的新信息,这反过来可能对设计更有效和更具选择性的缓激肽拮抗剂有价值。我们的研究结果似乎支持了其他人关于大鼠子宫和血管中存在不同亚型B₂受体的假说。

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