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时间治疗学和分子钟:肿瘤学中的临床意义。

Chronotherapy and the molecular clock: Clinical implications in oncology.

机构信息

INSERM, Villejuif, France.

出版信息

Adv Drug Deliv Rev. 2010 Jul 31;62(9-10):979-1001. doi: 10.1016/j.addr.2010.06.002. Epub 2010 Jun 23.

Abstract

The circadian timing system drives daily rhythmic changes in drug metabolism and controls rhythmic events in cell cycle, DNA repair, apoptosis, and angiogenesis in both normal tissue and cancer. Rodent and human studies have shown that the toxicity and anticancer activity of common cancer drugs can be significantly modified by the time of administration. Altered sleep/activity rhythms are common in cancer patients and can be disrupted even more when anticancer drugs are administered at their most toxic time. Disruption of the sleep/activity rhythm accelerates cancer growth. The complex circadian time-dependent connection between host, cancer and therapy is further impacted by other factors including gender, inter-individual differences and clock gene polymorphism and/or down regulation. It is important to take circadian timing into account at all stages of new drug development in an effort to optimize the therapeutic index for new cancer drugs. Better measures of the individual differences in circadian biology of host and cancer are required to further optimize the potential benefit of chronotherapy for each individual patient.

摘要

生物钟系统驱动药物代谢的日常节律变化,并控制正常组织和癌症中细胞周期、DNA 修复、细胞凋亡和血管生成的节律事件。啮齿动物和人体研究表明,常见癌症药物的毒性和抗癌活性可以通过给药时间显著改变。癌症患者常见睡眠/活动节律改变,甚至在抗癌药物在最具毒性的时间给药时,这种节律会被打乱。睡眠/活动节律的破坏会加速癌症的生长。宿主、癌症和治疗之间复杂的、依赖于时间的相互关系还受到其他因素的影响,包括性别、个体差异、时钟基因多态性和/或下调。在新药开发的所有阶段都考虑生物钟计时非常重要,这有助于优化新癌症药物的治疗指数。需要更好地衡量宿主和癌症生物钟生物学个体差异的措施,以进一步优化每个个体患者的时间治疗的潜在益处。

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