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金属响应调节蛋白对非天然酶的激活作用。

Unnatural enzyme activation by a metal-responsive regulatory protein.

作者信息

Halfin Olga, Avram Liat, Albeck Shira, Unger Tamar, Motiei Leila, Margulies David

机构信息

Department of Chemical and Structural Biology, Weizmann Institute of Science Rehovot Israel

Department of Chemical Research Support, Weizmann Institute of Science Rehovot Israel.

出版信息

Chem Sci. 2024 Aug 5;15(35):14209-17. doi: 10.1039/d4sc02635g.

Abstract

As a result of calcium ion binding, the calcium-dependent regulatory protein calmodulin (CaM) undergoes a conformational change, enabling it to bind to and activate a variety of enzymes. However, the detoxification enzyme glutathione -transferase (GST) is notably not among the enzymes activated by CaM. In this study, we demonstrate the feasibility of establishing, , an artificial regulatory link between CaM and GST using bifunctional chemical transducer (CT) molecules possessing binders for CaM and GST. We show that the CTs convert the constitutively active GST into a triggerable enzyme whose activity is unnaturally regulated by the CaM conformational state and consequently, by the level of calcium ions. The ability to reconfigure the regulatory function of CaM demonstrates a novel mode by which CTs could be employed to mediate artificial protein crosstalk, as well as a new means to achieve artificial control of enzyme activity by modulating the coordination of metal ions. Within this study, we also investigated the impact of covalent interaction between the CTs and the enzyme target. This investigation offers further insights into the mechanisms governing the function of CTs and the possibility of rendering them isoform specific.

摘要

由于钙离子结合,钙依赖性调节蛋白钙调蛋白(CaM)会发生构象变化,使其能够结合并激活多种酶。然而,解毒酶谷胱甘肽 - 转移酶(GST)显然不在被CaM激活的酶之列。在本研究中,我们证明了使用具有CaM和GST结合剂的双功能化学传感器(CT)分子在CaM和GST之间建立人工调节联系的可行性。我们表明,CT将组成型活性GST转化为一种可触发的酶,其活性受到CaM构象状态的非自然调节,进而受到钙离子水平的调节。重新配置CaM调节功能的能力展示了一种新的模式,通过该模式CT可用于介导人工蛋白质串扰,以及通过调节金属离子配位来实现对酶活性进行人工控制的新方法。在本研究中,我们还研究了CT与酶靶点之间共价相互作用的影响。这项研究为控制CT功能的机制以及使其具有亚型特异性的可能性提供了进一步的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f5b9/11389473/10fb311371d5/d4sc02635g-f1.jpg

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