Literature DB >> 26507796

Targeting DNA repair, DNA metabolism and replication stress as anti-cancer strategies.

Jordi Carreras Puigvert1, Kumar Sanjiv1, Thomas Helleday1.   

Abstract

Anti-cancer therapies targeting and damaging the DNA have been extensively used in the last 50 years since the discovery of nitrogen mustards, antimetabolites and platin agents. The use of these drugs is often limited by dose-limiting side effects related to their poor specificity. In recent years, much effort has been put on the discovery and development of compounds that would exploit defects in DNA repair in cancer cells such as Wee1, Chk1 or PARP1 inhibitors. However, not all cancers respond to these inhibitors. Recently, new developments towards specifically targeting broader characteristics of cancer such as replication stress (RS) and lost redox homeostasis have emerged. Oncogenes induce proliferation signals, which also result in replication-associated DNA damage, i.e. RS. Our knowledge into overall causes of RS, lesions produced and how these are signalled in cells to activate cell cycle checkpoints is evolving. Inhibition of ATR, which would normally keep non-deleterious levels of RS, induces intolerable RS levels for cancer cells. Interestingly, links between replication and transcription appear to underlie RS along with a reduction of the dNTP pool. Remarkably, sanitization of the dNTP pool by MutT homologue 1, impeding incorporation of oxidized dNTPs into the DNA, seems to be crucial for cancer cell survival. In this minireview we present an overview of current and novel strategies to target DNA repair and exploit DNA damage to treat cancer. We present the current models for cancer-associated RS as well as cancer phenotypic lethality. Both strategies are poised to better target cancer cells and reduce side effects.
© 2015 FEBS.

Entities:  

Keywords:  DNA damage; DNA metabolism; anti-cancer therapy; oncogenic stress; replication stress

Mesh:

Substances:

Year:  2015        PMID: 26507796     DOI: 10.1111/febs.13574

Source DB:  PubMed          Journal:  FEBS J        ISSN: 1742-464X            Impact factor:   5.542


  54 in total

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Review 9.  Recent Advances of Cell-Cycle Inhibitor Therapies for Pediatric Cancer.

Authors:  Christopher C Mills; E A Kolb; Valerie B Sampson
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