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预测细胞溶质磺基转移酶代谢药物的区域选择性。

Predicting Regioselectivity of Cytosolic Sulfotransferase Metabolism for Drugs.

机构信息

Cambridge Innovation Park, Optibrium Limited, Denny End Road, Cambridge CB25 9GL, U.K.

School of Chemistry, North Haugh, University of St Andrews, St Andrews KY16 9ST, U.K.

出版信息

J Chem Inf Model. 2023 Jun 12;63(11):3340-3349. doi: 10.1021/acs.jcim.3c00275. Epub 2023 May 25.

Abstract

Cytosolic sulfotransferases (SULTs) are a family of enzymes responsible for the sulfation of small endogenous and exogenous compounds. SULTs contribute to the conjugation phase of metabolism and share substrates with the uridine 5'-diphospho-glucuronosyltransferase (UGT) family of enzymes. UGTs are considered to be the most important enzymes in the conjugation phase, and SULTs are an auxiliary enzyme system to them. Understanding how the regioselectivity of SULTs differs from that of UGTs is essential from the perspective of developing novel drug candidates. We present a general ligand-based SULT model trained and tested using high-quality experimental regioselectivity data. The current study suggests that, unlike other metabolic enzymes in the modification and conjugation phases, the SULT regioselectivity is not strongly influenced by the activation energy of the rate-limiting step of the catalysis. Instead, the prominent role is played by the substrate binding site of SULT. Thus, the model is trained only on steric and orientation descriptors, which mimic the binding pocket of SULT. The resulting classification model, which predicts whether a site is metabolized, achieved a Cohen's kappa of 0.71.

摘要

细胞质硫转移酶(SULTs)是一类负责小内源性和外源性化合物磺化的酶。SULTs 参与代谢的结合相,与尿苷 5'-二磷酸葡萄糖醛酸基转移酶(UGT)家族的酶共享底物。UGTs 被认为是结合相最重要的酶,而 SULTs 是它们的辅助酶系统。从开发新的候选药物的角度来看,了解 SULT 与 UGT 的区域选择性差异至关重要。我们提出了一种基于配体的通用 SULT 模型,该模型使用高质量的实验区域选择性数据进行训练和测试。本研究表明,与修饰和结合相中其他代谢酶不同,SULT 的区域选择性不受催化限速步骤的活化能的强烈影响。相反,SULT 的底物结合位点起着突出的作用。因此,该模型仅在模拟 SULT 结合口袋的空间和取向描述符上进行训练。预测某个部位是否代谢的分类模型达到了 Cohen's kappa 为 0.71。

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