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DNA-dependent protein kinase promotes DNA end processing by MRN and CtIP.

SCIENCE ADVANCE. 2020; 
Deshpande RA, Myler LR, Soniat MM, Makharashvili N, Lee L, Lees-Miller SP, Finkelstein IJ,, Paull TT.
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Custom Vector Construction Proteins were detected using rabbit anti-FLAG, rabbit anti–DNA-PKcs, and mouse anti-His (GenScript) antibodies as well as streptavidin– Alexa Fluor 680 conjugateusing an Odyssey imager (Li-Cor) Get A Quote

摘要

The repair of DNA double-strand breaks occurs through nonhomologous end joining or homologous recombination in vertebrate cells-a choice that is thought to be decided by a competition between DNA-dependent protein kinase (DNA-PK) and the Mre11/Rad50/Nbs1 (MRN) complex but is not well understood. Using ensemble biochemistry and single-molecule approaches, here, we show that the MRN complex is dependent on DNA-PK and phosphorylated CtIP to perform efficient processing and resection of DNA ends in physiological conditions, thus eliminating the competition model. Endonucleolytic removal of DNA-PK-bound DNA ends is also observed at double-strand break sites in human cells. The involvement of DNA-PK in MRN-mediated e... More

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