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The development of pyrrolobenzodiazepines as antitumour agents.

机译:吡咯并苯二氮卓类药物作为抗肿瘤药的发展。

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INTRODUCTION: DNA interacting agents play a major role in cancer chemotherapy, either as single agents, in combination drug regimens, or as components of novel targeted therapies. The search for more selective and efficacious drugs that can deliver critical DNA damage with minimal side effects continues. AREAS COVERED: The development of the pyrrolobenzodiazepines (PBDs) from their discovery as natural products in the 1960s, through synthetic PBD monomers, PBD hybrids and conjugates, and PBD dimers is described. The latter molecules are capable of forming sequence selective, non-distorting and potently cytotoxic DNA interstrand cross-links in the minor groove of DNA. In particular, the development of PBD dimer SJG-136 (SG2000), currently in Phase II clinical trials, is presented. Potential future cancer therapeutic applications of PBDs, including their use as components of targeting strategies, are also discussed. EXPERT OPINION: The culmination of over four decades of study on structure-activity relationships of PBDs has led to a detailed understanding of how to introduce structural modification to enhance biological activity and potency. The challenge for the next phase in the development of the PBDs is to harness this activity and potency in a new generation of cancer therapeutics.
机译:引言:DNA相互作用剂在癌症化疗中起着主要作用,既可以作为单一药物,也可以作为联合药物方案,也可以作为新型靶向疗法的组成部分。仍在继续寻找更具选择性和功效的药物,这些药物可以对DNA造成严重损害,且副作用最小。涵盖的领域:描述了吡咯并苯并二氮杂卓(PBD)的发展,从其在1960年代作为天然产物被发现,通过合成的PBD单体,PBD杂化物和结合物以及PBD二聚体。后者的分子能够在DNA的小沟中形成序列选择性,无畸变和强细胞毒性的DNA链间交联。特别是,介绍了目前处于II期临床试验中的PBD二聚体SJG-136(SG2000)的开发。还讨论了PBD未来潜在的癌症治疗应用,包括其作为靶向策略的组成部分。专家意见:对PBD的结构-活性关系进行了四十多年研究的高潮,使人们对如何引入结构修饰以增强生物活性和效力有了更深入的了解。 PBD开发下一阶段的挑战是在新一代癌症治疗剂中利用这种活性和效力。

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