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Structural Insights into the Recognition of Mono- and Diacetylated Histones by the ATAD2B Bromodomain

J Med Chem. 2020-11; 
Jonathan T Lloyd , Kyle McLaughlin , Mulu Y Lubula , Jamie C Gay , Andrea Dest , Cong Gao , Margaret Phillips , Marco Tonelli , Gabriel Cornilescu , Matthew R Marunde , Chiara M Evans 1 , Samuel P Boyson , Samuel Carlson , Michael-Christopher Keogh , John L Markley , Seth Frietze , Karen C Glass
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Peptide Synthesis Histone peptides for other studies were either synthesized by the Peptide Core Facility at the University of Colorado Denver, GenScript, Get A Quote

摘要

Bromodomains exhibit preferences for specific patterns of post-translational modifications on core and variant histone proteins. We examined the ligand specificity of the ATAD2B bromodomain and compared it to its closely related paralogue in ATAD2. We show that the ATAD2B bromodomain recognizes mono- and diacetyllysine modifications on histones H4 and H2A. A structure-function approach was used to identify key residues in the acetyllysine-binding pocket that dictate the molecular recognition process, and we examined the binding of an ATAD2 bromodomain inhibitor by ATAD2B. Our analysis demonstrated that critical contacts required for bromodomain inhibitor coordination are conserved between the ATAD2/B bromodomai... More

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