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Multivalent binding of the hub protein LC8 at a newly discovered site in 53BP1

Biophys J. 2022-11; 
Jesse Howe, Austin Weeks, Patrick Reardon, Elisar Barbar
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Custom Vector Construction … coli in a pET24d expression vector (purchased from GenScript). To abolish LC8 binding, the three anchor residues for each QT site were mutated to AAA amino acids using New … Get A Quote

摘要

Tumor suppressor p53 binding protein 1 (53BP1) is a scaffolding protein involved in poly-ADP ribose polymerase inhibitor hypersensitivity in BRCA1-negative cancers. 53BP1 plays a critical role in the DNA damage response and relies on its oligomerization to create foci that promote repair of DNA double-strand breaks. Previous work shows that mutation of either the oligomerization domain or the dynein light chain 8 (LC8)-binding sites of 53BP1 results in reduced accumulation of 53BP1 at double-strand breaks. Mutation of both abolishes focus formation almost completely. Here, we show that, contrary to current literature, 53BP1 contains three LC8-binding sites, all of which are conserved in mammals. Isothermal titr... More

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