Phage Mu Gam protein promotes NHEJ in concert withEscherichia coliligase

Author:

Bhattacharyya Sudipta,Soniat Michael M.,Walker David,Jang Sooin,Finkelstein Ilya J.ORCID,Harshey Rasika M.

Abstract

The Gam protein of transposable phage Mu is an ortholog of eukaryotic and bacterial Ku proteins, which carry out nonhomologous DNA end joining (NHEJ) with the help of dedicated ATP-dependent ligases. Many bacteria carry Gam homologs associated with either complete or defective Mu-like prophages, but the role of Gam in the life cycle of Mu or in bacteria is unknown. Here, we show that MuGam is part of a two-component bacterial NHEJ DNA repair system. Ensemble and single-molecule experiments reveal that MuGam binds to DNA ends, slows the progress of RecBCD exonuclease, promotes binding of NAD+-dependentEscherichia coliligase A, and stimulates ligation. In vivo, Gam equally promotes both precise and imprecise joining of restriction enzyme-digested linear plasmid DNA, as well as of a double-strand break (DSB) at an engineered I-SceI site in the chromosome. Cell survival after the induced DSB is specific to the stationary phase. In long-term growth competition experiments, particularly upon treatment with a clastogen, the presence ofgamin a Mu lysogen confers a distinct fitness advantage. We also show that the role of Gam in the life of phage Mu is related not to transposition but to protection of genomic Mu copies from RecBCD when viral DNA packaging begins. Taken together, our data show that MuGam provides bacteria with an NHEJ system and suggest that the resulting fitness advantage is a reason that bacteria continue to retain thegamgene in the absence of an intact prophage.

Funder

HHS | NIH | National Institute of General Medical Sciences

HHS | NIH | National Cancer Institute

Welch Foundation

American Cancer Society

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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