On the Rational Design of Cooperative Receptors.

IF 10.4 1区 生物学 Q1 BIOPHYSICS
Gabriel Ortega, Alejandro Chamorro-Garcia, Francesco Ricci, Kevin W Plaxco
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引用次数: 4

Abstract

Cooperativity (homotropic allostery) is the primary mechanism by which evolution steepens the binding curves of biomolecular receptors to produce more responsive input-output behavior in biomolecular systems. Motivated by the ubiquity with which nature employs this effect, over the past 15 years we, together with other groups, have engineered this mechanism into several otherwise noncooperative receptors. These efforts largely aimed to improve the utility of such receptors in artificial biotechnologies, such as synthetic biology and biosensors, but they have also provided the first quantitative, experimental tests of longstanding ideas about the mechanisms underlying cooperativity. In this article, we review the literature on the design of this effect, paying particular attention to the design strategies involved, the extent to which each can be rationally applied to (and optimized for) new receptors, and what each teaches us about the origins and optimization of this important phenomenon.

论合作受体的合理设计。
协同性(同向变构)是进化使生物分子受体结合曲线变陡,从而在生物分子系统中产生更灵敏的输入-输出行为的主要机制。在自然界普遍使用这种效应的激励下,在过去的15年里,我们与其他团队一起,将这种机制设计成几种不合作的受体。这些努力主要是为了提高这些受体在人工生物技术中的效用,如合成生物学和生物传感器,但它们也为长期存在的关于合作机制的想法提供了第一次定量的实验测试。在本文中,我们回顾了关于这种效应设计的文献,特别关注所涉及的设计策略,每种策略可以合理地应用于(并优化)新受体的程度,以及每种策略教给我们的关于这一重要现象的起源和优化的知识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Annual Review of Biophysics
Annual Review of Biophysics 生物-生物物理
CiteScore
21.00
自引率
0.00%
发文量
25
期刊介绍: The Annual Review of Biophysics, in publication since 1972, covers significant developments in the field of biophysics, including macromolecular structure, function and dynamics, theoretical and computational biophysics, molecular biophysics of the cell, physical systems biology, membrane biophysics, biotechnology, nanotechnology, and emerging techniques.
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