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Modeling cellular pharmacokinetics of 14- and 15-membered macrolides with physicochemical properties

机译:具有物理化学性质的14和15元大环内酯类药物的药代动力学建模

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Macrolides with 14- and 15-membered ring are characterized by high and extensive tissue distribution, as well as good cellular accumulation and retention. Since macrolide structures do not fit the Lipinski rule of five, macrolide pharmacokinetic properties cannot be successfully predicted by common models based on data for small molecules. Here we describe the development of the first models for macrolide cellular pharmacokinetics. By comparison of cellular accumulation and retention in six human primary cell cultures of leukocytic and lung origin, as well as in lung carcinoma cell line NCI-H292, this cell line was found to be an adequate representative cell type for modeling macrolide cellular pharmacokinetics. Accumulation and retention in the NCI-H292 cells, as well as various physicochemical properties, were determined for a set of 48 rationally designed basic macrolide compounds. Classification models for predicting macrolide cellular accumulation and retention were developed using relatively easily determined and conceptually simple descriptors: experimentally determined physicochemical parameters ChromlogD and CHI IAM, as well as a calculated number of positively charged atoms (POS). The models were further tested and improved by addition of 37 structurally diverse macrolide molecules.
机译:具有14和15元环的大环内酯类药物的特点是组织分布广泛,高度分布,并具有良好的细胞蓄积和保留能力。由于大环内酯的结构不符合5的Lipinski规则,因此通用模型无法基于小分子数据成功预测大环内酯的药代动力学特性。在这里,我们描述了大环内酯细胞药代动力学的第一个模型的开发。通过比较白细胞和肺起源的六种人类原代细胞培养物中以及肺癌细胞系NCI-H292中的细胞蓄积和保留,发现该细胞系是用于建模大环内酯类药物药代动力学的适当代表性细胞类型。对于一组48种合理设计的基本大环内酯类化合物,确定了它们在NCI-H292细胞中的积累和保留以及各种理化特性。使用相对容易确定且概念上简单的描述符开发了预测大环内酯类细胞积累和保留的分类模型:实验确定的理化参数ChromlogD和CHI IAM,以及计算出的带正电原子数(POS)。通过添加37种结构多样的大环内酯分子,对模型进行了进一步测试和改进。

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