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癌症细胞的致命组合:用于药物发现的合成致死筛选。

A lethal combination for cancer cells: synthetic lethality screenings for drug discovery.

机构信息

Fondazione IFOM, IFOM-IEO Campus, via Adamello 16, 20139 Milan, Italy.

出版信息

Eur J Cancer. 2010 Nov;46(16):2889-95. doi: 10.1016/j.ejca.2010.07.031. Epub 2010 Aug 17.

Abstract

In recent years, cancer drug discovery has faced the challenging task of integrating the huge amount of information coming from the genomic studies with the need of developing highly selective target-based strategies within the context of tumour cells that experience massive genome instability. The combination between genetic and genomic technologies has been extremely useful and has contributed to efficiently transfer certain approaches typical of basic science to drug discover projects. An example comes from the synthetic lethal approaches, very powerful procedures that employ the rational used by geneticists working on model organisms. Applying the synthetic lethality (SL) screenings to anticancer therapy allows exploiting the typical features of tumour cells, such as genome instability, without changing them, as opposed to the conventional anticancer strategies that aim at counteracting the oncogenic signalling pathways. Recent and very encouraging clinical studies clearly show that certain promising anticancer compounds work through a synthetic lethal mechanism by targeting pathways that are specifically essential for the viability of cancer cells but not of normal cells. Herein we describe the rationale of the synthetic lethality approaches and the potential applications for anticancer therapy.

摘要

近年来,癌症药物研发面临着一项艰巨的任务,即需要将来自基因组研究的大量信息与在经历大规模基因组不稳定性的肿瘤细胞中开发高度选择性基于靶标的策略的需求相结合。遗传和基因组技术的结合非常有用,并有助于将某些典型的基础科学方法有效地转化为药物发现项目。一个例子来自于合成致死方法,这是一种非常强大的程序,它利用了遗传学家在模式生物上的合理方法。将合成致死(SL)筛选应用于抗癌治疗可以利用肿瘤细胞的典型特征,如基因组不稳定性,而不改变它们,与旨在对抗致癌信号通路的传统抗癌策略相反。最近非常令人鼓舞的临床研究清楚地表明,某些有前途的抗癌化合物通过靶向对癌细胞存活至关重要但对正常细胞不重要的途径的合成致死机制发挥作用。本文描述了合成致死方法的基本原理及其在抗癌治疗中的潜在应用。

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