4.5 Review Book Chapter

Base excision repair and its implications to cancer therapy

Journal

GUARDIANS OF THE GENOME: DNA DAMAGE AND REPAIR
Volume 64, Issue 5, Pages 831-843

Publisher

PORTLAND PRESS LTD
DOI: 10.1042/EBC20200013

Keywords

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Funding

  1. North West Cancer Research Career Development Fellowship [CDF2019.05]
  2. North West Cancer Research [CR1145, CR1197]

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Base excision repair (BER) has evolved to preserve the integrity of DNA following cellular oxidative stress and in response to exogenous insults. The pathway is a coordinated, sequential process involving 30 proteins or more in which single strand breaks are generated as intermediates during the repair process. While deficiencies in BER activity can lead to high mutation rates and tumorigenesis, cancer cells often rely on increased BER activity to tolerate oxidative stress. Targeting BER has been an attractive strategy to overwhelm cancer cells with DNA damage, improve the efficacy of radiotherapy and/or chemotherapy, or form part of a lethal combination with a cancer specific mutation/loss of function. We provide an update on the progress of inhibitors to enzymes involved in BER, and some of the challenges faced with targeting the BER pathway.

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