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设计肽表面活性剂稳定多种功能膜蛋白。

Designer peptide surfactants stabilize diverse functional membrane proteins.

机构信息

Center for Biomedical Engineering, Massachusetts Institute of Technology, NE47, 500 Technology Square, Cambridge, MA 02139-4307, USA.

出版信息

Chem Soc Rev. 2012 Mar 7;41(5):1721-8. doi: 10.1039/c1cs15180k. Epub 2011 Nov 15.

Abstract

Multi-spanning integral membrane proteins, including G-protein coupled receptors (GPCR), ion channels, and ion transporters, comprise a major class of drug targets. However, despite their vital importance, most molecular structures of membrane proteins remain elusive. This is largely due to lack of effective materials and methods to stabilize their functional conformation for sufficient time. Thus finding optimal surfactants and developing new approaches to study fundamental properties of unstable membrane proteins is urgently needed. In this tutorial review we summarize designer peptides with surfactant properties and their usefulness to stabilize membrane proteins. These peptide surfactants present new opportunities for the stabilization and characterization of diverse membrane proteins. Previous studies on the interaction between surfactant peptides and membrane proteins revealed strategies to design new peptides tailor-made for the stabilization of specific proteins. We review examples of solubilization, purification, long-term stabilization of membrane proteins, and the design principles of peptide sequences. We discuss future trends for exploiting spatial features, thermodynamic parameters, and self-assembling properties to create peptide surfactant structures to facilitate the characterization of diverse membrane proteins.

摘要

多跨整合膜蛋白,包括 G 蛋白偶联受体(GPCR)、离子通道和离子转运蛋白,构成了药物靶点的主要类别。然而,尽管它们至关重要,但大多数膜蛋白的分子结构仍然难以捉摸。这主要是由于缺乏有效稳定其功能构象的材料和方法,时间不够长。因此,迫切需要找到最佳的表面活性剂并开发新的方法来研究不稳定膜蛋白的基本特性。在本教程综述中,我们总结了具有表面活性剂特性的设计肽及其在稳定膜蛋白方面的有用性。这些肽表面活性剂为稳定和表征多种膜蛋白提供了新的机会。以前关于表面活性剂肽与膜蛋白相互作用的研究揭示了设计针对特定蛋白质稳定的新肽的策略。我们综述了用于溶解、纯化、长期稳定膜蛋白以及肽序列设计原理的示例。我们讨论了利用空间特征、热力学参数和自组装特性来创建肽表面活性剂结构以促进多种膜蛋白表征的未来趋势。

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