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蛋白质上过渡金属交换的细胞动力学:配位化学的挑战与机遇。

Cellular Dynamics of Transition Metal Exchange on Proteins: A Challenge but a Bonanza for Coordination Chemistry.

机构信息

Alternative Energies and Atomic Energy Commission-Fundamental Research Division-Interdisciplinary Research Institute of Grenoble (CEA-IRIG), University of Grenoble Alpes, F-38000 Grenoble, France.

National Institute of Health and Medical Research, University of Grenoble Alpes, Inserm U1055, F-38000 Grenoble, France.

出版信息

Biomolecules. 2020 Nov 21;10(11):1584. doi: 10.3390/biom10111584.

Abstract

Transition metals interact with a large proportion of the proteome in all forms of life, and they play mandatory and irreplaceable roles. The dynamics of ligand binding to ions of transition metals falls within the realm of Coordination Chemistry, and it provides the basic principles controlling traffic, regulation, and use of metals in cells. Yet, the cellular environment stands out against the conditions prevailing in the test tube when studying metal ions and their interactions with various ligands. Indeed, the complex and often changing cellular environment stimulates fast metal-ligand exchange that mostly escapes presently available probing methods. Reducing the complexity of the problem with purified proteins or in model organisms, although useful, is not free from pitfalls and misleading results. These problems arise mainly from the absence of the biosynthetic machinery and accessory proteins or chaperones dealing with metal / metal groups in cells. Even cells struggle with metal selectivity, as they do not have a metal-directed quality control system for metalloproteins, and serendipitous metal binding is probably not exceptional. The issue of metal exchange in biology is reviewed with particular reference to iron and illustrating examples in patho-physiology, regulation, nutrition, and toxicity.

摘要

过渡金属与所有生命形式中的大部分蛋白质相互作用,并且它们发挥着强制性和不可替代的作用。配体与过渡金属离子结合的动力学属于配位化学的范畴,它为控制金属在细胞中的运输、调节和利用提供了基本原理。然而,在研究金属离子及其与各种配体的相互作用时,细胞环境与试管中存在的条件明显不同。事实上,复杂且经常变化的细胞环境刺激了快速的金属-配体交换,而目前可用的探测方法大多无法捕捉到这种交换。用纯化的蛋白质或在模式生物中简化问题虽然有用,但也并非没有陷阱和误导性的结果。这些问题主要源于缺乏涉及细胞中金属/金属基团的生物合成机制和辅助蛋白或伴侣蛋白。即使是细胞也难以选择金属,因为它们没有针对金属蛋白的金属导向质量控制系统,偶然的金属结合可能也并不罕见。本文特别参考铁,综述了生物学中金属交换的问题,并举例说明了病理生理学、调控、营养和毒性等方面的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/202b/7700505/926b20d26f63/biomolecules-10-01584-g001.jpg

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