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The role of the efflux transporter, P-glycoprotein, at the blood-brain barrier in drug discovery

机译:外排转运蛋白P-糖蛋白在血脑屏障中的作用在药物发现中的作用

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摘要

The blood-brain barrier (BBB) expresses a high abundance of transporters, particularly P-glycoprotein (P-gp), that regulate endogenous and exogenous molecule uptake and removal of waste. This review discusses key drug metabolism and pharmacokinetic considerations for the efflux transporter P-gp at the BBB in drug discovery and development. We highlight the differences in P-gp expression and protein levels across species but the limited observations of species-specific substrates. Given the impact of age and disease on BBB biology, we summarise the modulation of P-gp for several neurological disorders and ageing and exemplify several disease-specific hurdles or opportunities for drug exposure in the brain. Furthermore, the review includes observations of CNS-related drug-drug interactions due to the inhibition or induction of P-gp at the BBB in animal studies and humans and the need for continued evaluation especially for compounds with a narrow therapeutic window. This review focusses primarily on small molecules but also considers the impact of new chemical entities, particularly beyond Ro5 molecules and their potential to be recognised as P-gp substrates as well as advanced drug delivery systems which offer an alternative approach to achieve and sustain central nervous system exposure.
机译:血脑屏障 (BBB) 表达大量转运蛋白,特别是 P-糖蛋白 (P-gp),调节内源性和外源性分子摄取和废物清除。本综述讨论了药物发现和开发中BBB外排转运蛋白P-gp的关键药物代谢和药代动力学考虑因素。我们强调了不同物种之间P-gp表达和蛋白质水平的差异,但对物种特异性底物的观察有限。鉴于年龄和疾病对 BBB 生物学的影响,我们总结了 P-gp 对几种神经系统疾病和衰老的调节作用,并举例说明了大脑中药物暴露的几种疾病特异性障碍或机会。此外,该综述还观察了由于动物研究和人类中 BBB 处 P-gp 的抑制或诱导而导致的 CNS 相关药物相互作用,以及需要继续评估,特别是对于治疗窗口较窄的化合物。本综述主要关注小分子,但也考虑了新化学实体的影响,特别是Ro5分子以外的影响,以及它们被公认为P-gp底物的潜力,以及先进的药物递送系统,这些系统为实现和维持中枢神经系统暴露提供了另一种方法。

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