Author: Hammel, Michal; Tainer, John A.
Title: Xâ€ray scattering reveals disordered linkers and dynamic interfaces in complexes and mechanisms for DNA doubleâ€strand break repair impacting cell and cancer biology Cord-id: 5qqaqeh4 Document date: 2021_6_5
ID: 5qqaqeh4
Snippet: Evolutionary selection ensures specificity and efficiency in dynamic metastable macromolecular machines that repair DNA damage without releasing toxic and mutagenic intermediates. Here we examine nonâ€homologous end joining (NHEJ) as the primary conserved DNA doubleâ€strand break (DSB) repair process in human cells. NHEJ has exemplary key roles in networks determining the development, outcome of cancer treatments by DSBâ€inducing agents, generation of antibody and Tâ€cell receptor diversity,
Document: Evolutionary selection ensures specificity and efficiency in dynamic metastable macromolecular machines that repair DNA damage without releasing toxic and mutagenic intermediates. Here we examine nonâ€homologous end joining (NHEJ) as the primary conserved DNA doubleâ€strand break (DSB) repair process in human cells. NHEJ has exemplary key roles in networks determining the development, outcome of cancer treatments by DSBâ€inducing agents, generation of antibody and Tâ€cell receptor diversity, and innate immune response for RNA viruses. We determine mechanistic insights into NHEJ structural biochemistry focusing upon advanced small angle Xâ€ray scattering (SAXS) results combined with Xâ€ray crystallography (MX) and cryoâ€electron microscopy (cryoâ€EM). SAXS coupled to atomic structures enables integrated structural biology for objective quantitative assessment of conformational ensembles and assemblies in solution, intraâ€molecular distances, structural similarity, functional disorder, conformational switching, and flexibility. Importantly, NHEJ complexes in solution undergo larger allosteric transitions than seen in their cryoâ€EM or MX structures. In the longâ€range synaptic complex, Xâ€ray repair crossâ€complementing 4 (XRCC4) plus XRCC4â€likeâ€factor (XLF) form a flexible bridge and linchpin for DNA ends bound to KU heterodimer (Ku70/80) and DNAâ€PKcs (DNAâ€dependent protein kinase catalytic subunit). Upon binding two DNA ends, autoâ€phosphorylation opens DNAâ€PKcs dimer licensing NHEJ via concerted conformational transformations of XLFâ€XRCC4, XLF–Ku80, and LigIV(BRCT)–Ku70 interfaces. Integrated structures reveal multifunctional roles for disordered linkers and modular dynamic interfaces promoting DSB end processing and alignment into the shortâ€range complex for ligation by LigIV. Integrated findings define dynamic assemblies fundamental to designing separationâ€ofâ€function mutants and allosteric inhibitors targeting conformational transitions in multifunctional complexes.
Search related documents:
Co phrase search for related documents- Try single phrases listed below for: 1
Co phrase search for related documents, hyperlinks ordered by date