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Modulation and absorption of xenobiotics: The synergistic role of CYP450 and P-gp activities in cancer and neurodegenerative disorders

机译:异源生物的调节和吸收:CYP450和P-gp活性在癌症和神经退行性疾病中的协同作用

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摘要

P-glycoprotein (P-gp) is involved in MDR and in neurodegenerative disorders such as Parkinson disease (PD), Alzheimer disease (AD) and epilepsy. Cytochrome P450 enzymes (CYP450s) catalyze the metabolism of a wide variety of endogenous and exogenous compounds including xenobiotics, drugs, environmental toxins, steroids, and fatty acids. P-gp substrates, inhibitors and inducers should be designed and developed studying interacting mechanism with both P-gp an CYP450 enzymes before they could be employed in MDR and/or in neurodegenerative disorders. Here, the ex vivo rat everted gut sac assay has been proposed as an immediate approach to simultaneously study metabolism and transport of drugs. Elacridar, verapamil and cyclosporine A (CsA), P-gp inhibitor, substrate and modulator respectively, have been tested to validate this ex vivo approach. The new model have been used yet to develop our ligands MC18, MC266 and MC80, both as potential drugs for MDR and radiotracers for diagnosis of neurodegenerative disorders. Herein, a comparative evaluation of transport and metabolic results, by using in vitro, ex vivo and in vivo assays, is reported.
机译:P-糖蛋白(P-gp)参与MDR和神经退行性疾病,例如帕金森氏病(PD),阿尔茨海默氏病(AD)和癫痫病。细胞色素P450酶(CYP450s)催化多种内源性和外源性化合物的代谢,包括异种生物,药物,环境毒素,类固醇和脂肪酸。在设计P-gp底物,抑制剂和诱导剂之前,应先研究它们与P-gp和CYP450酶的相互作用机理,然后才能将其用于MDR和/或神经退行性疾病。在此,已提出离体大鼠外翻肠囊测定法作为同时研究药物代谢和转运的直接方法。分别测试了Elacridar,维拉帕米和环孢素A(CsA),P-gp抑制剂,底物和调节剂,以验证这种离体方法。新模型尚未用于开发我们的配体MC18,MC266和MC80,它们既可作为MDR的潜在药物,也可作为放射性示踪剂用于诊断神经退行性疾病。本文中,报道了通过使用体外,离体和体内测定法对转运和代谢结果的比较评价。

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