首页> 外文期刊>Journal of Medicinal Chemistry >Quantitative Assessment of the Impact of Fluorine Substitution on P-Glycoprotein (P-gp) Mediated Efflux, Permeability, Lipophilicity, and Metabolic Stability
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Quantitative Assessment of the Impact of Fluorine Substitution on P-Glycoprotein (P-gp) Mediated Efflux, Permeability, Lipophilicity, and Metabolic Stability

机译:氟取代对P-糖蛋白(P-gp)介导的流出,通透性,亲脂性和代谢稳定性的影响的定量评估

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摘要

Strategic replacement of one or more hydrogen atoms with fluorine atom(s) is a common tactic to improve potency at a given target and/or to modulate parameters such as metabolic stability and pK(a) Molecular weight (MW) is a key parameter in design, and incorporation of fluorine is associated with a disproportionate increase in MW considering the van der Waals radius of fluorine versus hydrogen. Herein we examine a large compound data set to understand the effect of introducing fluorine on the risk of encountering P-glycoprotein mediated efflux (as measured by MDR efflux ratio), passive permeability, lipophilicity, and metabolic stability. Statistical modeling of the MDR ER data demonstrated that an increase in MW as a result of introducing fluorine atoms does not lead to higher risk of P-gp mediated efflux. Fluorine-corrected molecular weight (MWFC), where the molecular weight of fluorine has been subtracted, was found to be a more relevant descriptor.
机译:用氟原子战略性地取代一个或多个氢原子是提高给定目标效能和/或调节代谢稳定性和pK(a)等参数的常用策略。分子量(MW)是考虑到氟相对于氢的范德华半径,氟的设计和掺入与MW的不成比例的增加有关。本文中,我们检查了一个大型化合物数据集,以了解引入氟对遭遇P-糖蛋白介导的外排率(通过MDR外排率测量),被动通透性,亲脂性和代谢稳定性的影响。 MDR ER数据的统计模型表明,由于引入氟原子而导致的分子量增加不会导致P-gp介导的外排风险增加。发现氟校正分子量(MWFC)(其中减去了氟的分子量)是更相关的描述。

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