Small-molecule inhibitors identify the RAD52-ssDNA interaction as critical for recovery from replication stress and for survival of BRCA2 deficient cells

Sarah R. Hengel; Eva Malacaria; Laura Folly da Silva Constantino; Fletcher E. Bain; Andrea Diaz; Brandon G Koch; Liping Yu; Meng Wu; Pietro Pichierri; M. Ashley Spies; Maria Spies

doi:https://doi.org/10.7554/elife.14740

doi.org/10.7554/elife.14740

Small-molecule inhibitors identify the RAD52-ssDNA interaction as critical for recovery from replication stress and for survival of BRCA2 deficient cells

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..., Maria Spies

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eLife7.70

Volume: 5

Published: Jul 19, 2016

Abstract

The DNA repair protein RAD52 is an emerging therapeutic target of high importance for BRCA-deficient tumors. Depletion of RAD52 is synthetically lethal with defects in tumor suppressors BRCA1, BRCA2 and PALB2. RAD52 also participates in the recovery of the stalled replication forks. Anticipating that ssDNA binding activity underlies the RAD52 cellular functions, we carried out a high throughput screening campaign to identify compounds that...

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Paper Details

Title

Small-molecule inhibitors identify the RAD52-ssDNA interaction as critical for recovery from replication stress and for survival of BRCA2 deficient cells

DOI

doi.org/10.7554/elife.14740

Published Date

Jul 19, 2016

Journal

eLife

Volume

5

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