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来自莫氏矛头蝮蛇毒的P-I类金属蛋白酶是一种具有激肽原酶活性的脯氨酸后切割肽酶:对底物选择性和动力学行为的见解。

P-I class metalloproteinase from Bothrops moojeni venom is a post-proline cleaving peptidase with kininogenase activity: insights into substrate selectivity and kinetic behavior.

作者信息

Okamoto Débora N, Kondo Marcia Y, Oliveira Lilian C G, Honorato Rodrigo V, Zanphorlin Leticia M, Coronado Monika A, Araújo Mariana S, da Motta Guacyara, Veronez Camila L, Andrade Sheila S, Oliveira Paulo S L, Arni Raghuvir K, Cintra Adelia C O, Sampaio Suely V, Juliano Maria A, Juliano Luiz, Murakami Mário T, Gouvea Iuri E

机构信息

Departamento de Biofísica, Universidade Federal de São Paulo, 04044-020 São Paulo, SP, Brazil.

Laboratório Nacional de Biociências, Centro Nacional de Pesquisas em Energia e Materiais, 13083-100 Campinas, SP, Brazil.

出版信息

Biochim Biophys Acta. 2014 Mar;1844(3):545-52. doi: 10.1016/j.bbapap.2013.12.014. Epub 2013 Dec 27.

DOI:10.1016/j.bbapap.2013.12.014
PMID:24373874
Abstract

Snake venom metalloproteinases (SVMPs) belonging to P-I class are able to hydrolyze extracellular matrix proteins and coagulation factors triggering local and systemic reactions by multiple molecular mechanisms that are not fully understood. BmooMPα-I, a P-I class SMVP from Bothrops moojeni venom, was active upon neuro- and vaso-active peptides including angiotensin I, bradykinin, neurotensin, oxytocin and substance P. Interestingly, BmooMPα-I showed a strong bias towards hydrolysis after proline residues, which is unusual for most of characterized peptidases. Moreover, the enzyme showed kininogenase activity similar to that observed in plasma and cells by kallikrein. FRET peptide assays indicated a relative promiscuity at its S2-S'2 subsites, with proline determining the scissile bond. This unusual post-proline cleaving activity was confirmed by the efficient hydrolysis of the synthetic combinatorial library MCA-GXXPXXQ-EDDnp, described as resistant for canonical peptidases, only after Pro residues. Structural analysis of the tripeptide LPL complexed with BmooMPα-I, generated by molecular dynamics simulations, assisted in defining the subsites and provided the structural basis for subsite preferences such as the restriction of basic residues at the S2 subsite due to repulsive electrostatic effects and the steric impediment for large aliphatic or aromatic side chains at the S1 subsite. These new functional and structural findings provided a further understanding of the molecular mechanisms governing the physiological effects of this important class of enzymes in envenomation process.

摘要

属于P-I类的蛇毒金属蛋白酶(SVMPs)能够水解细胞外基质蛋白和凝血因子,通过多种尚未完全了解的分子机制引发局部和全身反应。BmooMPα-I是一种来自莫氏矛头蝮蛇毒的P-I类SMVP,对包括血管紧张素I、缓激肽、神经降压素、催产素和P物质在内的神经活性和血管活性肽具有活性。有趣的是,BmooMPα-I对脯氨酸残基后的水解表现出强烈的偏好,这对大多数已表征的肽酶来说是不寻常的。此外,该酶表现出与血浆和细胞中激肽释放酶观察到的类似的激肽原酶活性。荧光共振能量转移肽分析表明,其S2-S'2亚位点相对混杂,脯氨酸决定了可裂解键。只有在脯氨酸残基之后,合成组合文库MCA-GXXPXXQ-EDDnp(被描述为对典型肽酶具有抗性)的有效水解证实了这种不寻常的脯氨酸后切割活性。通过分子动力学模拟生成的与BmooMPα-I复合的三肽LPL的结构分析,有助于确定亚位点,并为亚位点偏好提供了结构基础,例如由于排斥性静电效应,S2亚位点对碱性残基的限制以及S1亚位点对大脂肪族或芳香族侧链的空间阻碍。这些新的功能和结构发现进一步了解了在蛇毒中毒过程中控制这类重要酶的生理效应的分子机制。

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