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Modulation of cis-diamminedichloroplatinum(II) resistance: a review

机译:顺二氨二氯铂(II)耐药性的调节:审查。

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In this review an inventory is made of agents used to circumvent cis-diamminedichloroplatinum(II) (CDDP) resistance in vitro and in vivo. Agents that affect CDDP accumulation and membrane related systems, cytoplasmic defense mechanisms, as well as DNA accessibility and repair are reviewed. In resistant cell lines that have decreased accumulation, this can be restored by hyperthermic treatment. With or without effects on accumulation compounds that affect cell signal transduction often increase CDDP cytotoxicity. Calcium channel blockers and calmodulin inhibitors do not seem to be uniformly good modulators of CDDP resistance. For transduction modulators as well as cellular calcium affecting agents mechanisms are mainly unclear or controversial. Glutathione appears, with the now available agents, to be the most promising target for modulation of cytoplasmic defense mechanisms. At the nuclear level the inhibition of DNA repair related enzymes as well as the use of modified nucleosides to interfere with repair is studied in various cell lines. Results with these agents suggest opportunities for clinically feasible cytotoxicity modulation. DNA accessibility could in vitro be affected, but seems to be an unreliable target for modulation. Whenever possible the resistance mechanism affected and the mode of action of the modulator are discussed. As an alternative for modulation another method of overcoming CDDP resistance namely the application of CDDP analogues is considered.
机译:在本综述中,列出了用于在体外和体内规避顺二氨二氯铂(II)(CDDP)耐药性的药物。审查影响CDDP积累和膜相关系统,细胞质防御机制以及DNA可达性和修复的因素。在具有减少的积累的抗性细胞系中,可以通过高温治疗来恢复。对蓄积有影响或没有影响,影响细胞信号转导的化合物通常会增加CDDP细胞毒性。钙通道阻滞剂和钙调蛋白抑制剂似乎并不是CDDP抗性的统一良好调节剂。对于转导调节剂以及细胞钙影响剂的机制主要尚不清楚或有争议。谷胱甘肽与现在可用的试剂一起,似乎是调节细胞质防御机制的最有希望的靶标。在核水平上,在各种细胞系中研究了对DNA修复相关酶的抑制以及修饰核苷的使用以干扰修复。这些药物的结果提示了临床上可行的细胞毒性调节的机会。 DNA的可及性在体外可能会受到影响,但似乎不是调节的可靠目标。只要有可能,就会讨论受影响的阻力机制和调制器的作用方式。作为调制的替代方法,考虑了另一种克服CDDP抗性的方法,即CDDP类似物的应用。

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