Structural study of wild-type and phospho-mimic XRCC4 dimer and multimer proteins using circular dichroism spectroscopy.
Kai NishikuboMaho HasegawaYudai IzumiKentaro FujiiKoichi MatsuoYoshihisa MatsumotoAkinari YokoyaPublished in: International journal of radiation biology (2023)
An increase in the β-strand content in XRCC4 is essential for stabilization of the multimeric form through C-terminal phosphorylation, allowing formation of the large double-strand break repair machinery.