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通过结构-活性分析揭示富含脯氨酸寡肽(Bj-PRO-10c)对心血管的作用:降压和心动过缓作用的分离。

Insights into cardiovascular effects of proline-rich oligopeptide (Bj-PRO-10c) revealed by structure-activity analyses: dissociation of antihypertensive and bradycardic effects.

机构信息

Special Laboratory of Applied Toxinology-CAT/Cepid, Butantan Institute, Av. Vital Brasil, 1500, Sao Paulo, SP, 05503-900, Brazil.

出版信息

Amino Acids. 2014 Feb;46(2):401-13. doi: 10.1007/s00726-013-1630-x. Epub 2013 Dec 14.

DOI:10.1007/s00726-013-1630-x
PMID:24337901
Abstract

We have previously reported that the proline-rich decapeptide from Bothrops jararaca (Bj-PRO-10c) causes potent and sustained antihypertensive and bradycardic effects in SHR. These activities are independent of ACE inhibition. In the present study, we used the Ala-scan approach to evaluate the importance of each amino acid within the sequence of Bj-PRO-10c (Pyr(1)-Asn(2)-Trp(3)-Pro(4)-His(5)-Pro(6)-Gln(7)-Ile(8)-Pro(9)-Pro(10)). The antihypertensive and bradycardic effects of the analogues Bj-PRO-10c Ala(3), Bj-PRO-10c Ala(7), Bj-PRO-10c Ala(8) were similar to those of Bj-PRO-10c, whereas the analogues Bj-PRO-10c Ala(2), Bj-PRO-10c Ala(4), Bj-PRO-10c Ala(5), Bj-PRO-10c Ala(9), and Bj-PRO-10c Ala(10) kept the antihypertensive activity and lost bradycardic activity considerably. In contrast, Bj-PRO-10c Ala(1) and Bj-PRO-10c Ala(6) were unable to provoke any cardiovascular activity. In summary, we demonstrated that (1) the Pyr(1) and Pro(6) residues are essential for both, the antihypertensive and bradycardic effects of Bj-PRO-10c; (2) Ala-scan approach allowed dissociating blood pressure reduction and bradycardic effects. Conformational properties of the peptides were examined by means of circular dichroism (CD) spectroscopy. The different Ala-scan analogues caused either an increase or decrease in the type II polyproline helix content compared to Bj-PRO-10c. The complete loss of activity of the Pro(6) → Ala(6) mutant is probably due to the fact that in the parent peptide the His(5)-Pro(6) bond can exist in the cis configuration, which could correspond to the conformation of this bond in the bound state. Current data support the Bj-PRO-10c as a promising leader prototype to develop new agents to treat cardiovascular diseases and its co-morbidities.

摘要

我们之前曾报道过,来自矛头蝮蛇(Bothrops jararaca)的脯氨酸丰富的十肽(Bj-PRO-10c)可引起 SHR 产生强大而持久的降压和心率降低作用。这些活性与 ACE 抑制无关。在本研究中,我们使用 Ala 扫描方法来评估 Bj-PRO-10c 序列中每个氨基酸的重要性(Pyr(1)-Asn(2)-Trp(3)-Pro(4)-His(5)-Pro(6)-Gln(7)-Ile(8)-Pro(9)-Pro(10))。类似物 Bj-PRO-10c Ala(3)、Bj-PRO-10c Ala(7)、Bj-PRO-10c Ala(8)的降压和心率降低作用与 Bj-PRO-10c 相似,而类似物 Bj-PRO-10c Ala(2)、Bj-PRO-10c Ala(4)、Bj-PRO-10c Ala(5)、Bj-PRO-10c Ala(9)和 Bj-PRO-10c Ala(10)保持了降压活性,而大大降低了心率降低活性。相比之下,Bj-PRO-10c Ala(1)和 Bj-PRO-10c Ala(6)均不能引起任何心血管活动。总之,我们证明了(1)Pyr(1)和 Pro(6)残基对于 Bj-PRO-10c 的降压和心率降低作用都是必需的;(2)Ala 扫描方法允许分离血压降低和心率降低作用。通过圆二色性(CD)光谱检查了肽的构象性质。与 Bj-PRO-10c 相比,不同的 Ala 扫描类似物引起的 II 型聚脯氨酸螺旋含量增加或减少。Pro(6)→Ala(6)突变体完全失去活性可能是由于在母体肽中,His(5)-Pro(6)键可以存在顺式构型,这可能对应于该键在结合状态下的构象。当前的数据支持将 Bj-PRO-10c 作为开发用于治疗心血管疾病及其合并症的新型药物的有前途的先导原型。

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