Isoxazole-Derived Amino Acids are Bromodomain-Binding Acetyl-Lysine Mimics: Incorporation into Histone H4 Peptides and Histone H3.

Abad-Zapatero; Allfrey; Arrowsmith; Brand; Chalker; Chatterjee; Choudhary; Choudhary; Dancy; De Luca; Dhall; Falorni; Fatkins; Filippakopoulos; Filippakopoulos; Gallenkamp; Hay; Hewings; Hewings; Hirsch; Hirsch; Huang; Jamonnak; Jamonnak; Jenuwein; Jung; Kouzarides; Muir; Neumann; Neumann; Philpott; Sanchez; Sharp; Simon; Smith; Smith; Strahl; Tessarz; Weinert

Isoxazole-Derived Amino Acids are Bromodomain-Binding Acetyl-Lysine Mimics: Incorporation into Histone H4 Peptides and Histone H3.

Authors: Abad-Zapatero
Allfrey
Arrowsmith
Brand
Chalker
Chatterjee
Choudhary
Choudhary
Dancy
De Luca
Dhall
Falorni
Fatkins
Filippakopoulos
Filippakopoulos
Gallenkamp
Hay
Hewings
Hewings
Hirsch
Hirsch
Huang
Jamonnak
Jamonnak
Jenuwein
Jung
Kouzarides
Muir
Neumann
Neumann
Philpott
Sanchez
Sharp
Simon
Smith
Smith
Strahl
Tessarz
Weinert
Publication date: 6 June 2016
Publisher: Angew Chem Int Ed Engl
Doi

Abstract

A range of isoxazole-containing amino acids was synthesized that displaced acetyl-lysine-containing peptides from the BAZ2A, BRD4(1), and BRD9 bromodomains. Three of these amino acids were incorporated into a histone H4-mimicking peptide and their affinity for BRD4(1) was assessed. Affinities of the isoxazole-containing peptides are comparable to those of a hyperacetylated histone H4-mimicking cognate peptide, and demonstrated a dependence on the position at which the unnatural residue was incorporated. An isoxazole-based alkylating agent was developed to selectively alkylate cysteine residues in situ. Selective monoalkylation of a histone H4-mimicking peptide, containing a lysine to cysteine residue substitution (K12C), resulted in acetyl-lysine mimic incorporation, with high affinity for the BRD4 bromodomain. The same technology was used to alkylate a K18C mutant of histone H3.Pfizer Neusentis for studentship suppor