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The structural basis for partitioning of the XRCC1/DNA ligase III-α BRCT-mediated dimer complexes.

Nucleic Acids Res.. 2011-09; 
Matthew J. Cuneo, Scott A. Gabel, Joseph M. Krahn, Melissa A. Ricker, and Robert E. London. National Institute of Environmental Health Sciences, NIH, DHHS, Research Triangle Park, NC, USA.
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摘要

The ultimate step common to almost all DNA repair pathways is the ligation of the nicked intermediate to form contiguous double-stranded DNA. In the mammalian nucleotide and base excision repair pathways, the ligation step is carried out by ligase III-α. For efficient ligation, ligase III-α is constitutively bound to the scaffolding protein XRCC1 through interactions between the C-terminal BRCT domains of each protein. Although structural data for the individual domains has been available, no structure of the complex has been determined and several alternative proposals for this interaction have been advanced. Interpretation of the models is complicated by the formation of homodimers that, depending... More

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