Norman C.W. Wong scite author profile

Increased synthesis of Apolipoprotein A-I (ApoA-I) and HDL is believed to provide a new approach to treating atherosclerosis through the stimulation of reverse cholesterol transport. RVX-208 increases the production of ApoA-I in hepatocytes in vitro, and in vivo in monkeys and humans, which results in increased HDL-C, but the molecular target was not previously reported. Using binding assays and X-ray crystallography, we now show that RVX-208 selectively binds to bromodomains of the BET (Bromodomain and Extra Terminal) family, competing for a site bound by the endogenous ligand, acetylated lysine, and that this accounts for its pharmacological activity. siRNA experiments further suggest that induction of ApoA-I mRNA is mediated by BET family member BRD4. These data indicate that RVX-208 increases ApoA-I production through an epigenetic mechanism and suggests that BET inhibition may be a promising new approach to the treatment of atherosclerosis.

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Complement Is an Essential Component of the Immune Response to Adeno-Associated Virus Vectors

Zaiss¹,

Cotter

White

et al. 2008

J Virol

135

132

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Norman C.W. Wong

Differential Activation of Innate Immune Responses by Adenovirus and Adeno-Associated Virus Vectors

Advances in Our Understanding of Thyroid Hormone Action at the Cellular Level*

BET inhibition blocks inflammation-induced cardiac dysfunction and SARS-CoV-2 infection

RVX-208, an Inducer of ApoA-I in Humans, Is a BET Bromodomain Antagonist

Complement Is an Essential Component of the Immune Response to Adeno-Associated Virus Vectors

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