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The interaction of bortezomib with multidrug transporters: implications for therapeutic applications in advanced multiple myeloma and other neoplasias

机译:硼替佐米与多种药物转运蛋白的相互作用:对晚期多发性骨髓瘤和其他瘤形成的治疗应用的意义。

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摘要

PurposeBortezomib is an important agent in multiple myeloma treatment, but resistance in cell lines and patients has been described. The main mechanisms of resistance described in cancer fall into one of two categories, pharmacokinetic resistance (PK), e.g. over expression of drug efflux pumps and pharmacodynamic resistance, e.g. apoptosis resistance or altered survival pathways, where the agent reaches an appropriate concentration, but this fails to propagate an appropriate cell death response. Of the known pump mechanisms, P-glycoprotein (P-gp) is the best studied and considered to be the most important in contributing to general PK drug resistance. Resistance to bortezomib is multifactorial and there are conflicting indications that cellular overexpression of P-gp may contribute to resistance agent. Hence, better characterization of the interactions of this drug with classical resistance mechanisms should identify improved treatment applications.
机译:目的硼替佐米是多发性骨髓瘤治疗中的重要药物,但已经描述了细胞系和患者的耐药性。癌症中描述的耐药性的主要机制属于以下两类之一:药代动力学耐药性(PK),例如药物外排泵的过度表达和药效抗性,例如凋亡抗药性或改变的存活途径,其中药剂达到适当的浓度,但这不能传播适当的细胞死亡反应。在已知的泵浦机制中,对P-糖蛋白(P-gp)的研究最为深入,被认为对促成一般PK药物耐药性最重要。对硼替佐米的抗药性是多因素的,并且有相互矛盾的迹象表明,P-gp的细胞过表达可能与抗药性有关。因此,更好地表征这种药物与经典耐药机制的相互作用应该可以识别出改善的治疗应用。

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