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Targeting base excision repair to improve cancer therapies

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journal contribution
posted on 2007-11-19, 16:53 authored by Ricky A. Sharma, Grigory L. Dianov
Most commonly used cancer therapies, particularly ionizing radiation and certain classes of cytotoxic chemotherapies, cause cell death by damaging DNA. Base excision repair (BER) is the major system responsible for the removal of corrupt DNA bases and repair of DNA single strand breaks generated spontaneously and induced by exogenous DNA damaging factors such as certain cancer therapies. In this review, the physico-chemical properties of the proteins involved in BER are discussed with particular emphasis on molecular mechanisms coordinating repair processes. The aim of this review is to apply extensive knowledge that currently exists regarding the biochemical mechanisms involved in human BER to the molecular biology of current therapies for cancer. It is anticipated that the application of this knowledge will translate into the development of novel effective therapies for improving existing treatments such as radiation therapy and oxaliplatin chemotherapy.

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Citation

Molecular Aspects of Medicine, 2007, 28, pp.345-374

Published in

Molecular Aspects of Medicine

Publisher

Elsevier

Available date

2007-11-19

Publisher version

http://www.sciencedirect.com/science/article/pii/S0098299707000568

Notes

This is the authors' final draft of the paper published as Molecular Aspects of Medicine, 2007, 28, pp. 345-374. The final definitive version is available from www.sciencedirect.com, doi:10.1016/j.mam.2007.06.002.

Language

en

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