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金属对内含肽剪接的影响:综述。

Metal effect on intein splicing: A review.

机构信息

School of Biotechnology, Kalinga Institute of Industrial Technology, Bhubaneswar, Odisha, 751024, India.

School of Biotechnology, Kalinga Institute of Industrial Technology, Bhubaneswar, Odisha, 751024, India.

出版信息

Biochimie. 2021 Jun;185:53-67. doi: 10.1016/j.biochi.2021.03.006. Epub 2021 Mar 13.

Abstract

Inteins are intervening polypeptides that interrupt the functional domains of several important proteins across the three domains of life. Inteins excise themselves from the precursor protein, ligating concomitant extein residues in a process called protein splicing. Post-translational auto-removal of inteins remain critical for the generation of active proteins. The perspective of inteins in science is a robust field of research, however fundamental studies centralized upon splicing regulatory mechanism are imperative for addressing more intricate issues. Controlled engineering of intein splicing has many applications; intein inhibition can facilitate novel drug design, while activation of intein splicing is exploited in protein purification. This paper provides a comprehensive review of the past and recent advances in the splicing regulation via metal-intein interaction. We compare the behavior of different metal ions on diverse intein systems. Though metals such as Zn, Cu, Pt, Cd, Co, Ni exhibit intein inhibitory effect heterogeneously on different inteins, divalent metal ions such as Ca and Mg fail to do so. The observed diversity in the metal-intein interaction arises mostly due to intein polymorphism and variations in atomic structure of metals. A mechanistic understanding of intein regulation by metals in native as well as synthetically engineered intein systems may yield potent intein inhibitors via direct or indirect approach.

摘要

内肽是介入的多肽,它们中断了生命的三个领域中几种重要蛋白质的功能域。内肽从前体蛋白中自我切除,同时将伴随的外显肽残基连接起来,这个过程称为蛋白质剪接。内肽的翻译后自动去除对于产生活性蛋白质仍然至关重要。内肽在科学中的观点是一个强大的研究领域,然而,集中研究剪接调控机制对于解决更复杂的问题是必要的。内肽剪接的受控工程有许多应用;内肽抑制可以促进新型药物设计,而内肽剪接的激活则被用于蛋白质纯化。本文全面回顾了通过金属-内肽相互作用进行剪接调控的过去和最新进展。我们比较了不同金属离子对内肽系统的影响。虽然 Zn、Cu、Pt、Cd、Co、Ni 等金属对内肽的抑制作用在不同的内肽系统中表现出不均匀性,但 Ca 和 Mg 等二价金属离子则没有这种作用。金属-内肽相互作用的多样性主要归因于内肽的多态性和金属原子结构的变化。对天然和合成工程化内肽系统中金属对内肽调控的机制理解,可能通过直接或间接的方法产生有效的内肽抑制剂。

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