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通过结构重建与催化能力相结合来评估叶酸介导的一碳途径中关键酶的作用机制。

Pairing structural reconstruction with catalytic competence to evaluate the mechanisms of key enzymes in the folate-mediated one-carbon pathway.

机构信息

Department of Clinical Sciences, Lund University, Malmö, Sweden.

出版信息

FEBS J. 2023 May;290(9):2279-2291. doi: 10.1111/febs.16439. Epub 2022 Mar 31.

Abstract

Mammalian metabolism comprises a series of interlinking pathways that include two major cycles: the folate and methionine cycles. The folate-mediated metabolic cycle uses several oxidation states of tetrahydrofolate to carry activated one-carbon units to be readily used and interconverted within the cell. They are required for nucleotide synthesis, methylation and metabolism, and particularly for proliferation of cancer cells. Based on the latest progress in genome-wide CRISPR loss-of-function viability screening of 789 cell lines, we focus on the most cancer-dependent enzymes in this pathway, especially those that are hyperactivated in cancer, to provide new insight into the chemical basis for cancer drug development. Since the complete 3D structure of several of these enzymes of the one-carbon pathway in their active form are not available, we used homology modelling integrated with the interpretation of the reaction mechanism. In addition, have reconstructed the most likely scenario for the reactions taking place paired with their catalytic competence that provides a testable framework for this pathway.

摘要

哺乳动物代谢包括一系列相互关联的途径,其中包括两个主要循环:叶酸和蛋氨酸循环。叶酸介导的代谢循环利用四氢叶酸的几种氧化态将活化的一碳单位带入细胞内,以便于使用和相互转化。它们是核苷酸合成、甲基化和代谢所必需的,特别是癌细胞的增殖所必需的。基于对 789 种细胞系进行全基因组范围的 CRISPR 功能丧失性存活筛选的最新进展,我们专注于该途径中最依赖于癌症的酶,特别是那些在癌症中过度激活的酶,为癌症药物开发的化学基础提供新的见解。由于这些一碳途径中的几种酶的完整 3D 结构在其活性形式下尚不可用,因此我们使用同源建模与反应机制的解释相结合。此外,我们还重建了最有可能发生的反应与它们的催化能力配对的情况,为该途径提供了一个可测试的框架。

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