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随机集合、构象自适应协作和酶解毒。

Stochastic ensembles, conformationally adaptive teamwork, and enzymatic detoxification.

机构信息

Department of Medicinal Chemistry and Department of Applied Mathematics, University of Washington, Seattle, Washington 98190, United States.

出版信息

Biochemistry. 2011 May 17;50(19):3866-72. doi: 10.1021/bi200275r. Epub 2011 Apr 20.

Abstract

It has been appreciated for a long time that enzymes exist as conformational ensembles throughout multiple stages of the reactions they catalyze, but there is renewed interest in the functional implications. The energy landscape that results from conformationlly diverse poteins is a complex surface with an energetic topography in multiple dimensions, even at the transition state(s) leading to product formation, and this represents a new paradigm. At the same time there has been renewed interest in conformational ensembles, a new paradigm concerning enzyme function has emerged, wherein catalytic promiscuity has clear biological advantages in some cases. "Useful", or biologically functional, promiscuity or the related behavior of "multifunctionality" can be found in the immune system, enzymatic detoxification, signal transduction, and the evolution of new function from an existing pool of folded protein scaffolds. Experimental evidence supports the widely held assumption that conformational heterogeneity promotes functional promiscuity. The common link between these coevolving paradigms is the inherent structural plasticity and conformational dynamics of proteins that, on one hand, lead to complex but evolutionarily selected energy landscapes and, on the other hand, promote functional promiscuity. Here we consider a logical extension of the overlap between these two nascent paradigms: functionally promiscuous and multifunctional enzymes such as detoxification enzymes are expected to have an ensemble landscape with more states accessible on multiple time scales than substrate specific enzymes. Two attributes of detoxification enzymes become important in the context of conformational ensembles: these enzymes metabolize multiple substrates, often in substrate mixtures, and they can form multiple products from a single substrate. These properties, combined with complex conformational landscapes, lead to the possibility of interesting time-dependent, or emergent, properties. Here we demonstrate these properties with kinetic simulations of nonequilibrium steady state (NESS) behavior resulting from energy landscapes expected for detoxification enzymes. Analogous scenarios with other promiscuous enzymes may be worthy of consideration.

摘要

长期以来,人们一直认为酶在其催化的反应的多个阶段都以构象集合体的形式存在,但现在人们对其功能意义又重新产生了兴趣。从构象多样性的蛋白质中产生的能量景观是一个复杂的表面,即使在通向产物形成的过渡态(多个维度)也具有能量地形,这代表了一个新的范例。与此同时,人们对构象集合体重新产生了兴趣,一个新的酶功能范例已经出现,其中催化的多功能性在某些情况下具有明显的生物学优势。在某些情况下,“有用的”或具有生物学功能的多功能性或相关的“多功能性”行为可以在免疫系统、酶解毒、信号转导以及从现有折叠蛋白质支架库中进化出新功能中找到。实验证据支持了这样一种广泛持有的假设,即构象异质性促进了功能的多功能性。这些共同进化范例之间的共同联系是蛋白质固有的结构可塑性和构象动力学,一方面导致了复杂但经过进化选择的能量景观,另一方面促进了功能的多功能性。在这里,我们考虑了这两个新兴范例之间重叠的逻辑扩展:解毒酶等具有功能多样性和多功能性的酶预计将具有可在多个时间尺度上访问更多状态的集合景观,而不是具有底物特异性的酶。在构象集合体的背景下,解毒酶的两个属性变得很重要:这些酶代谢多种底物,通常是在底物混合物中,并且它们可以从单个底物中形成多种产物。这些特性与复杂的构象景观相结合,导致了有趣的时间依赖性或涌现的特性的可能性。在这里,我们通过对预期用于解毒酶的能量景观的非平衡稳态(NESS)行为的动力学模拟来证明这些特性。其他多功能酶的类似情况可能值得考虑。

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Enzyme promiscuity: a mechanistic and evolutionary perspective.酶的多功能性:一种机制和进化的观点。
Annu Rev Biochem. 2010;79:471-505. doi: 10.1146/annurev-biochem-030409-143718.

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