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抗冻蛋白药物:活性的结构要求。

Antifreeze glycoprotein agents: structural requirements for activity.

机构信息

Escuela de Alimentos, Pontificia Universidad Católica de Valparaíso (PUCV), Valparaíso, Chile.

出版信息

J Sci Food Agric. 2011 Nov;91(14):2507-10. doi: 10.1002/jsfa.4473. Epub 2011 Jul 1.

Abstract

Antifreeze glycoproteins (AFGPs) are considered to be the most efficient means to reduce ice damage to cell tissues since they are able to inhibit growth and crystallization of ice. The key element of antifreeze proteins is to act in a non-colligative manner which allows them to function at concentrations 300-500 times lowers than other dissolved solutes. During the past decade, AFGPs have demonstrated tremendous potential for many pharmaceutical and food applications. Presently, the only route to obtain AFGPs involves the time consuming and expensive process of isolation and purification from deep-sea polar fishes. Unfortunately, it is not amenable to mass production and commercial applications. The lack of understanding of the mechanism through which the AFGPs inhibit ice growth has also hampered the realization of industrial and biotechnological applications. Here we report the structural motifs that are essential for antifreeze activity of AFGPs, and propose a unified mechanism based on both recent studies of short alanine peptides and structure activity relationship of synthesized AFGPs.

摘要

抗冻蛋白 (AFGPs) 被认为是降低细胞组织冰损伤的最有效方法,因为它们能够抑制冰的生长和结晶。抗冻蛋白的关键要素是以非依数性方式发挥作用,从而使它们能够在比其他溶解溶质低 300-500 倍的浓度下发挥作用。在过去的十年中,AFGPs 在许多药物和食品应用中显示出巨大的潜力。目前,获得 AFGPs 的唯一途径是从深海极地鱼类中耗时且昂贵的分离和纯化过程。不幸的是,它不适用于大规模生产和商业应用。对抗冻蛋白抑制冰生长机制的理解不足也阻碍了工业和生物技术应用的实现。在这里,我们报告了 AFGPs 抗冻活性所必需的结构基序,并基于近期对短丙氨酸肽的研究和合成 AFGPs 的结构活性关系提出了一个统一的机制。

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