EBioMedicine (Nov 2015)

BET Bromodomain Blockade Mitigates Intimal Hyperplasia in Rat Carotid Arteries

  • Bowen Wang,
  • Mengxue Zhang,
  • Toshio Takayama,
  • Xudong Shi,
  • Drew Alan Roenneburg,
  • K. Craig Kent,
  • Lian-Wang Guo

DOI
https://doi.org/10.1016/j.ebiom.2015.09.045
Journal volume & issue
Vol. 2, no. 11
pp. 1650 – 1661

Abstract

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Background: Intimal hyperplasia is a common cause of many vasculopathies. There has been a recent surge of interest in the bromo and extra-terminal (BET) epigenetic “readers” including BRD4 since the serendipitous discovery of JQ1(+), an inhibitor specific to the seemingly undruggable BET bromodomains. The role of the BET family in the development of intimal hyperplasia is not known. Methods: We investigated the effect of BET inhibition on intimal hyperplasia using a rat balloon angioplasty model. Results: While BRD4 was dramatically up-regulated in the rat and human hyperplastic neointima, blocking BET bromodomains with JQ1(+) diminished neointima in rats. Knocking down BRD4 with siRNA, or treatment with JQ1(+) but not the inactive enantiomer JQ1(−), abrogated platelet-derived growth factor (PDGF-BB)-stimulated proliferation and migration of primary rat aortic smooth muscle cells. This inhibitory effect of JQ1(+) was reproducible in primary human aortic smooth muscle cells. In human aortic endothelial cells, JQ1(+) prevented cytokine-induced apoptosis and impairment of cell migration. Furthermore, either BRD4 siRNA or JQ1(+) but not JQ1(−), substantially down-regulated PDGF receptor-α which, in JQ1(+)-treated arteries versus vehicle control, was also reduced. Conclusions: Blocking BET bromodomains mitigates neointima formation, suggesting an epigenetic approach for effective prevention of intimal hyperplasia and associated vascular diseases.

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