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在溶组织梭菌胶原酶的切割位点设计含D-氨基酸的类胶原肽以实现对其的抑制

Engineering D-Amino Acid Containing Collagen Like Peptide at the Cleavage Site of Clostridium histolyticum Collagenase for Its Inhibition.

作者信息

Velmurugan Punitha, Jonnalagadda Raghava Rao, Nair Balachandran Unni

机构信息

Council of Scientific and Industrial Research-Central Leather Research Institute, Chemical Laboratory, Adyar, Chennai, 600 020, India.

出版信息

PLoS One. 2015 May 14;10(5):e0124398. doi: 10.1371/journal.pone.0124398. eCollection 2015.

Abstract

Collagenase is an important enzyme which plays an important role in degradation of collagen in wound healing, cancer metastasis and even in embryonic development. However, the mechanism of this degradation has not yet been completely understood. In the field of biomedical and protein engineering, the design and development of new peptide based materials is of main concern. In the present work an attempt has been made to study the effect of DAla in collagen like peptide (imino-poor region of type I collagen) on the structure and stability of peptide against enzyme hydrolysis. Effect of replacement of DAla in the collagen like peptide has been studied using circular dichroic spectroscopy (CD). Our findings suggest that, DAla substitution leads to conformational changes in the secondary structure and favours the formation of polyproline II conformation than its L-counterpart in the imino-poor region of collagen like peptides. Change in the chirality of alanine at the cleavage site of collagenase in the imino-poor region inhibits collagenolytic activity. This may find application in design of peptides and peptidomimics for enzyme-substrate interaction, specifically with reference to collagen and other extra cellular matrix proteins.

摘要

胶原酶是一种重要的酶,在伤口愈合、癌症转移甚至胚胎发育过程中的胶原蛋白降解中发挥着重要作用。然而,这种降解的机制尚未完全被理解。在生物医学和蛋白质工程领域,新型肽基材料的设计与开发是主要关注点。在当前工作中,已尝试研究D - 丙氨酸在类胶原肽(I型胶原的贫亚氨基区域)中对肽的结构以及抗酶水解稳定性的影响。使用圆二色光谱法(CD)研究了类胶原肽中D - 丙氨酸取代的影响。我们的研究结果表明,在类胶原肽的贫亚氨基区域,D - 丙氨酸取代会导致二级结构的构象变化,并且比起其L - 对应物,更有利于聚脯氨酸II构象的形成。在贫亚氨基区域胶原酶切割位点处丙氨酸手性的改变会抑制胶原分解活性。这可能在用于酶 - 底物相互作用的肽和拟肽设计中找到应用,特别是涉及胶原蛋白和其他细胞外基质蛋白的情况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bda1/4431724/c252610810c4/pone.0124398.g001.jpg

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