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Structural role for DNA Ligase IV in promoting the fidelity of non-homologous end joining

Benjamin M. Stinson, Sean M. Carney, Johannes C. Walter () and Joseph J. Loparo ()
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Benjamin M. Stinson: Harvard Medical School
Sean M. Carney: Harvard Medical School
Johannes C. Walter: Harvard Medical School
Joseph J. Loparo: Harvard Medical School

Nature Communications, 2024, vol. 15, issue 1, 1-13

Abstract: Abstract Nonhomologous end joining (NHEJ), the primary pathway of vertebrate DNA double-strand-break (DSB) repair, directly re-ligates broken DNA ends. Damaged DSB ends that cannot be immediately re-ligated are modified by NHEJ processing enzymes, including error-prone polymerases and nucleases, to enable ligation. However, DSB ends that are initially compatible for re-ligation are typically joined without end processing. As both ligation and end processing occur in the short-range (SR) synaptic complex that closely aligns DNA ends, it remains unclear how ligation of compatible ends is prioritized over end processing. In this study, we identify structural interactions of the NHEJ-specific DNA Ligase IV (Lig4) within the SR complex that prioritize ligation and promote NHEJ fidelity. Mutational analysis demonstrates that Lig4 must bind DNA ends to form the SR complex. Furthermore, single-molecule experiments show that a single Lig4 binds both DNA ends at the instant of SR synapsis. Thus, Lig4 is poised to ligate compatible ends upon initial formation of the SR complex before error-prone processing. Our results provide a molecular basis for the fidelity of NHEJ.

Date: 2024
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DOI: 10.1038/s41467-024-45553-z

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