Loss of CHD1 causes DNA repair defects and enhances prostate cancer therapeutic responsiveness

The CHD1 gene, encoding the chromo‐domain helicase DNA‐binding protein‐1, is one of the most frequently deleted genes in prostate cancer. Here, we examined the role of CHD1 in DNA double‐strand break (DSB) repair in prostate cancer cells. We show that CHD1 is required for the recruitment of CtIP to...

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Published in:EMBO reports Vol. 17; no. 11; pp. 1609 - 1623
Main Authors: Kari, Vijayalakshmi, Mansour, Wael Yassin, Raul, Sanjay Kumar, Baumgart, Simon J, Mund, Andreas, Grade, Marian, Sirma, Hüseyin, Simon, Ronald, Will, Hans, Dobbelstein, Matthias, Dikomey, Ekkehard, Johnsen, Steven A
Format: Journal Article
Language:English
Published: London Blackwell Publishing Ltd 01-11-2016
Nature Publishing Group UK
John Wiley and Sons Inc
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Summary:The CHD1 gene, encoding the chromo‐domain helicase DNA‐binding protein‐1, is one of the most frequently deleted genes in prostate cancer. Here, we examined the role of CHD1 in DNA double‐strand break (DSB) repair in prostate cancer cells. We show that CHD1 is required for the recruitment of CtIP to chromatin and subsequent end resection during DNA DSB repair. Our data support a role for CHD1 in opening the chromatin around the DSB to facilitate the recruitment of homologous recombination (HR) proteins. Consequently, depletion of CHD1 specifically affects HR‐mediated DNA repair but not non‐homologous end joining. Together, we provide evidence for a previously unknown role of CHD1 in DNA DSB repair via HR and show that CHD1 depletion sensitizes cells to PARP inhibitors, which has potential therapeutic relevance. Our findings suggest that CHD1 deletion, like BRCA1/2 mutation in ovarian cancer, may serve as a marker for prostate cancer patient stratification and the utilization of targeted therapies such as PARP inhibitors, which specifically target tumors with HR defects. Synopsis Chromo‐domain helicase DNA‐binding protein‐1 (CHD1) promotes HR‐mediated DSB repair. The depletion of CHD1 enhances cellular sensitivity to PARP inhibitors, which has potential therapeutic implications for CHD1‐depleted prostate cancers. CHD1 is required for the recruitment of CtIP and efficient DNA DSB repair. CHD1 facilitates the opening of chromatin at DSB and promotes HR repair. CHD1 depletion elicits cellular sensitivity to PARP inhibition. Graphical Abstract Chromo‐domain helicase DNA‐binding protein‐1 (CHD1) promotes HR‐mediated DSB repair. The depletion of CHD1 enhances cellular sensitivity to PARP inhibitors, which has potential therapeutic implications for CHD1‐depleted prostate cancers.
Bibliography:ark:/67375/WNG-XV9J342S-8
ArticleID:EMBR201642352
National Overseas Scholarship, Government of India - No. 11015/49/2010-SCD-V
istex:CAD372749D8A6EE670632F58C59ECFFF026B9C10
Deutsche Forschungsgemeinschaft - No. GRK1034
Expanded View Figures PDFTable EV1Table EV2Table EV3Table EV4Table EV5Source Data for Expanded ViewReview Process FileSource Data for Figure 2C
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These authors contributed equally to this work
ISSN:1469-221X
1469-3178
DOI:10.15252/embr.201642352