Department of Chemistry, Washington State University, Pullman, Washington 99163, USA.
Mol Pharm. 2013 Apr 1;10(4):1262-8. doi: 10.1021/mp300568r. Epub 2013 Feb 13.
Metabolism by aldehyde oxidase (AO) has been responsible for a number of drug failures in clinical trials. The main reason is the clearance values for drugs metabolized by AO are underestimated by allometric scaling from preclinical species. Furthermore, in vitro human data also underestimates clearance. We have developed the first in silico models to predict both in vitro and in vivo human intrinsic clearance for 8 drugs with just two chemical descriptors. These models explain a large amount of the variance in the data using two computational estimates of the electronic and steric features of the reaction. The in vivo computational models for human metabolism are better than in vitro preclinical animal testing at predicting human intrinsic clearance. Thus, it appears that AO is amenable to computational prediction of rates, which may be used to guide drug discovery, and predict pharmacokinetics for clinical trials.
醛氧化酶(AO)代谢已导致许多临床试验中的药物失败。主要原因是,通过种属间的体表面积比例外推法,AO 代谢的药物清除率被低估。此外,体外人体数据也低估了清除率。我们已经开发出了第一个可以预测 8 种药物的体外和体内人体内在清除率的计算模型,仅使用了两个化学描述符。这些模型使用两个计算得出的反应电子和立体特征的估算值,解释了数据中大量的差异。用于预测人体代谢的体内计算模型比体外临床前动物测试更能预测人体内在清除率。因此,似乎 AO 可以进行计算预测,这可能用于指导药物发现,并预测临床试验的药代动力学。