Abstract
In a recent paper published in Cell Research, a cryo-EM structure reveals the interface between DNA-PKcs and the Ku70/80:DNA complex, together forming the DNA-dependent protein kinase holoenzyme in non-homologous DNA end joining. Insight from this structure suggests how an allosteric rearrangement of DNA-PKcs driven by Ku70/80:DNA binding regulates kinase activity in this largest member of a family of structurally homologous phosphoinositide 3-kinase-related protein kinases that includes mTOR, ATR, and ATM.
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CITATION STYLE
Watanabe, G., Lieber, M. R., & Williams, D. (2017, November 1). Structural step forward for NHEJ. Cell Research. Nature Publishing Group. https://doi.org/10.1038/cr.2017.119
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