Celgene Corp. , 10300 Campus Point Drive, Suite 100, San Diego, CA 92121 , USA +1 858 795 4991 ; +1 858 552 8775 ;
Expert Opin Drug Metab Toxicol. 2013 Dec;9(12):1597-612. doi: 10.1517/17425255.2013.834046. Epub 2013 Aug 31.
Fourteen drugs targeting protein kinases have been approved by the United States Food and Drug Administration (FDA) between the years 2000 and 2011. While the mechanisms of action and clinical data have been reported, the preclinical absorption, distribution, metabolism and elimination (ADME) data on these compounds are not readily available.
This review summarizes the structural, physicochemical and preclinical ADME properties of the 14 kinase inhibitors. For this purpose, the authors identified common preclinical ADME features of the majority of these inhibitors.
The authors believe engendering a combination of the following attributes will greatly improve one's chance of discovering kinase inhibitors with a successful development path: i) Lipinski Rule of Five and Veber's rules, ii) most basic pKa values ≤ 9, iii) low to moderate clearance values for each species and iv) moderate to high Caco-2 permeability. Furthermore, they recommend primarily focusing on in vitro hepatic stability and rodent in vivo disposition properties at early screening stage and using Caco-2 permeability/efflux ratio to salvage compounds with rapid rodent plasma clearance. In vitro drug-drug interaction data should be evaluated in the context of the dosing route, dosing regimen, elimination pathways, enzyme phenotyping profile, efficacious exposure and the target disease.
2000 年至 2011 年间,美国食品和药物管理局(FDA)批准了 14 种针对蛋白激酶的药物。虽然已经报道了这些药物的作用机制和临床数据,但这些化合物的临床前吸收、分布、代谢和消除(ADME)数据并不容易获得。
本综述总结了这 14 种激酶抑制剂的结构、物理化学和临床前 ADME 特性。为此,作者确定了这些抑制剂的大多数常见的临床前 ADME 特征。
作者认为,将以下属性相结合将极大地提高发现具有成功开发途径的激酶抑制剂的机会:i)利宾斯基五规则和韦伯规则,ii)大多数基本 pKa 值≤9,iii)每种物种的低至中等清除值,iv)中等至高的 Caco-2 渗透率。此外,他们建议在早期筛选阶段主要关注体外肝稳定性和啮齿动物体内处置特性,并使用 Caco-2 渗透率/外排比来挽救具有快速啮齿动物血浆清除率的化合物。应根据给药途径、给药方案、消除途径、酶表型特征、有效暴露和目标疾病来评估体外药物相互作用数据。
