ATM induces MacroD2 nuclear export upon DNA damage

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Abstract

ADP-ribosylation is a dynamic post-translation modification that regulates the early phase of various DNA repair pathways by recruiting repair factors to chromatin. ADP-ribosylation levels are defined by the activities of specific transferases and hydrolases. However, except for the transferase PARP1/ARDT1 little is known about regulation of these enzymes. We found that MacroD2, a mono-ADP-ribosylhydrolase, is exported from the nucleus upon DNA damage, and that this nuclear export is induced by ATM activity. We show that the export is dependent on the phosphorylation of two SQ/TQ motifs, suggesting a novel direct interaction between ATM and ADP-ribosylation. Lastly, we show that MacroD2 nuclear export temporally restricts its recruitment to DNA lesions, which may decrease the net ADP-ribosylhydrolase activity at the site of DNA damage. Together, our results identify a novel feedback regulation between two crucial DNA damage-induced signaling pathways: ADPribosylation and ATM activation.

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APA

Golia, B., Moeller, G. K., Jankevicius, G., Schmidt, A., Hegele, A., Preißer, J., … Timinszky, G. (2017). ATM induces MacroD2 nuclear export upon DNA damage. Nucleic Acids Research, 45(1), 244–254. https://doi.org/10.1093/nar/gkw904

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