首页> 外文期刊>British Journal of Cancer >Platinum and other metal coordination compounds in cancer chemotherapy. A commentary on the sixth international symposium: San Diego, California, 23-26th January 1991
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Platinum and other metal coordination compounds in cancer chemotherapy. A commentary on the sixth international symposium: San Diego, California, 23-26th January 1991

机译:铂和其他金属配位化合物在癌症化疗中的作用。第六届国际研讨会的评论:1991年1月23日至26日,加利福尼亚州圣地亚哥

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The use of molecular biological methodologies has provided a greater understanding of the cytotoxic effects of cisplatin and the underlying mechanisms of tumour cell resistance. Resistance to cisplatin is often multifocal with plasma membrane, cytosolic and nuclear components. Cisplatin-DNA adducts appear to be recognised by specific damage recognition proteins. Proteins associated with the transport of platinum through plasma membranes and genes associated with cisplatin resistance appear to be close to being elucidated. Current Phase I and Phase II clinical trials with platinum-containing complexes largely focus on the 1,2 diaminocyclohexane (DACH) carrier ligand, the dicarboxylatocyclobutane leaving group and complexes which circumvent cisplatin resistance in murine leukaemia models. At present, the trials are at too early a stage to allow comment on their clinical utility and, consequently, the relevance of the murine leukaemia-based preclinical observations. On the horizon, orally active platinum (IV) ammine/amine dicarboxylate dichloride coordination complexes with preclinical toxicological profiles similar to carboplatin should enter clinical trial in the next year.
机译:分子生物学方法的使用已使人们对顺铂的细胞毒性作用和肿瘤细胞耐药性的潜在机制有了更深入的了解。对顺铂的耐药性通常与质膜,胞质和核成分多灶。顺铂-DNA加合物似乎被特定的损伤识别蛋白识别。与铂通过质膜转运相关的蛋白质和与顺铂耐药性相关的基因似乎已接近阐明。当前的含铂配合物的I期和II期临床试验主要集中在1,2二氨基环己烷(DACH)载体配体,二羧基环戊烷离去基团和在鼠白血病模型中规避顺铂耐药性的配合物。目前,该试验尚处于早期阶段,尚不能评论其临床效用,因此不能发表基于鼠白血病的临床前观察结果的相关性。在不久的将来,具有类似于卡铂的临床前毒理学特征的口服活性氨(氨)/二羧酸二胺二氯化物配位化合物应在明年进入临床试验。

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