药物样性质和分数亲脂性指数作为联合度量

IF 3.4 Q2 CHEMISTRY, MEDICINAL ADMET and DMPK Pub Date : 2021-10-08 DOI:10.5599/admet.1022
A. Tsantili-Kakoulidou, V. Demopoulos
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引用次数: 8

摘要

分数脂性指数(FLI)是一种将对数P和对数D以加权方式结合起来的类似药物的复合指标。在本研究中,一个扩展的数据集证实了先前建立的药物样FLI范围为0-8,使用两种计算系统进行logP /log D评估,免费软件MedChem Designer和ClogP。根据吸收分数百分比(%FA)将数据集分为两类- 1类包括高至中等吸收水平的药物,2类包括吸收不良的药物。FLI和FLI- c(基于ClogP的FLI)类药物范围分别覆盖了92%和91%的1类药物。使用MlogP,建立了一个更窄的类似药物的FLI-M范围0-7,覆盖了91%的1类药物。研究了在FLI (FLI- c, FLI- m)类药物范围内电离程度对内在亲脂性的依赖,以及其他Ro5性质(Mw, HD, HA)之间的相互关系,以确定药物样/非药物样组合是候选药物优先考虑的单一性质的更安全选择。在这个意义上,我们提出了一个Mw和极性原子数量(Mw/NO)的组合度量来说明尺寸和极性。将50设为截止值,1类药物与2类药物的区别明显,超过70%的1类药物的Mw/NO>50,而2类药物的情况则相反。
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Drug-like Properties and Fraction Lipophilicity Index as a combined metric
Fraction Lipophicity Index (FLI) has been developed as a composite drug-like metric combining log P and log D in a weighted manner. In the present study, an extended data set confirmed the previously established drug-like FLI range 0-8 using two calculation systems for log P/log D assessment, the freeware MedChem Designer and ClogP. The dataset was split into two classes according to the percentage of fraction absorbed (%FA) - class 1 including drugs with high to medium absorption levels and class 2 including poorly absorbed drugs. The FLI and FLI-C (ClogP based FLI) drug-like range covers 92 % and 91 % of class 1 drugs, respectively. Using MlogP, a narrower drug-like FLI-M range 0-7 was established, covering 91 % of class 1 drugs. The dependence of the degree of ionization to intrinsic lipophilicity within the FLI (FLI-C, FLI-M) drug-like range as well as the inter-relation between the other Ro5 properties (Mw, HD, HA) was explored to define drug-like / non-drug-like combinations as a safer alternative to single properties for drug candidates’ prioritization. In this sense, we propose a combined metric of Mw and the number of polar atoms (Mw/NO) to account for both size and polarity. Setting the value 50 as cutoff, a distinct differentiation between class 1 and class 2 drugs was obtained with Mw/NO>50 for more than 70 % of class 1 drugs, while the opposite was observed for class 2 drugs.
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来源期刊
ADMET and DMPK
ADMET and DMPK Multiple-
CiteScore
4.40
自引率
0.00%
发文量
22
审稿时长
4 weeks
期刊介绍: ADMET and DMPK is an open access journal devoted to the rapid dissemination of new and original scientific results in all areas of absorption, distribution, metabolism, excretion, toxicology and pharmacokinetics of drugs. ADMET and DMPK publishes the following types of contributions: - Original research papers - Feature articles - Review articles - Short communications and Notes - Letters to Editors - Book reviews The scope of the Journal involves, but is not limited to, the following areas: - physico-chemical properties of drugs and methods of their determination - drug permeabilities - drug absorption - drug-drug, drug-protein, drug-membrane and drug-DNA interactions - chemical stability and degradations of drugs - instrumental methods in ADMET - drug metablic processes - routes of administration and excretion of drug - pharmacokinetic/pharmacodynamic study - quantitative structure activity/property relationship - ADME/PK modelling - Toxicology screening - Transporter identification and study
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