1. Academic Validation
  2. Suppression of inflammation by a synthetic histone mimic

Suppression of inflammation by a synthetic histone mimic

  • Nature. 2010 Dec 23;468(7327):1119-23. doi: 10.1038/nature09589.
Edwige Nicodeme 1 Kate L Jeffrey Uwe Schaefer Soren Beinke Scott Dewell Chun-Wa Chung Rohit Chandwani Ivan Marazzi Paul Wilson Hervé Coste Julia White Jorge Kirilovsky Charles M Rice Jose M Lora Rab K Prinjha Kevin Lee Alexander Tarakhovsky
Affiliations

Affiliation

  • 1 Centre de Recherche GSK, 27 Avenue du Québec, 91140 Villebon Sur Yvette, France.
Abstract

Interaction of pathogens with cells of the immune system results in activation of inflammatory gene expression. This response, although vital for immune defence, is frequently deleterious to the host due to the exaggerated production of inflammatory proteins. The scope of inflammatory responses reflects the activation state of signalling proteins upstream of inflammatory genes as well as signal-induced assembly of nuclear chromatin complexes that support mRNA expression. Recognition of post-translationally modified histones by nuclear proteins that initiate mRNA transcription and support mRNA elongation is a critical step in the regulation of gene expression. Here we present a novel pharmacological approach that targets inflammatory gene expression by interfering with the recognition of acetylated histones by the bromodomain and extra terminal domain (BET) family of proteins. We describe a synthetic compound (I-BET) that by 'mimicking' acetylated histones disrupts chromatin complexes responsible for the expression of key inflammatory genes in activated macrophages, and confers protection against lipopolysaccharide-induced endotoxic shock and bacteria-induced sepsis. Our findings suggest that synthetic compounds specifically targeting proteins that recognize post-translationally modified histones can serve as a new generation of immunomodulatory drugs.

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