Pharmacological inhibition of ABCA1 degradation increases HDL biogenesis and exhibits antiatherogenesis

Reijiro Arakawa,Maki Tsujita,Noriyuki Iwamoto,Chisato Ito-Ohsumi,Rui Lu,Chen-Ai Wu,Kenji Shimizu,Tomoji Aotsuka,Hashime Kanazawa,Sumiko Abe-Dohmae,Shinji Yokoyama

doi:10.1194/jlr.m900122-jlr200

Reijiro Arakawa, Maki Tsujita + Show 9 more

Open Access

https://doi.org/10.1194/jlr.m900122-jlr200

Copy DOI

Abstract

Expression of ABCA1 is regulated by transcription of the gene and calpain-mediated proteolytic degradation, and inhibition ABCA1 degradation results in increased ABCA1 and HDL biogenesis in vitro. We examined whether this approach could be a potential antiatherogenic treatment. Although probucol inhibits both the activity and degradation of ABCA1, its oxidized products, spiroquinone and diphenoquinone, reduce degradation of ABCA1 without inhibiting its activity or altering transcription of the ABCA1 gene. Accordingly, both compounds enhanced apolipoprotein A-I/ABCA1-dependent generation of HDL in vitro, and increased hepatic ABCA1 and plasma HDL without increasing antioxidant activity in plasma when given to rabbits. Both compounds also decreased vascular lipid deposition in cholesterol-fed rabbits. We therefore conclude that stabilization of ABCA1 against calpain-mediated degradation is a novel and potentially important strategy to increase HDL formation and prevent atherosclerosis. Spiroquinone and diphenoquinone are potential seeds for development of such drugs.

Highlights

Expression of ABCA1 is regulated by transcription of the gene and calpain-mediated proteolytic degradation, and inhibition ABCA1 degradation results in increased ABCA1 and HDL biogenesis in vitro
SQ, and DQ were incorporated into acetylated low density lipoprotein (acLDL) and fed to THP-1 macrophages and cellular lipid release by apolipoprotein A-I (apoA-I) was measured
ABCA1 protein was markedly increased by probucol in spite of inhibition of HDL formation, consistent with our previous finding [17] (Fig. 1B)