Macrophage Mitochondrial Energy Status Regulates Cholesterol Efflux and Is Enhanced by Anti-miR33 in Atherosclerosis

Circ Res. 2015 Jul 17;117(3):266-78. doi: 10.1161/CIRCRESAHA.117.305624. Epub 2015 May 22.

Abstract

Rationale: Therapeutically targeting macrophage reverse cholesterol transport is a promising approach to treat atherosclerosis. Macrophage energy metabolism can significantly influence macrophage phenotype, but how this is controlled in foam cells is not known. Bioinformatic pathway analysis predicts that miR-33 represses a cluster of genes controlling cellular energy metabolism that may be important in macrophage cholesterol efflux.

Objective: We hypothesized that cellular energy status can influence cholesterol efflux from macrophages, and that miR-33 reduces cholesterol efflux via repression of mitochondrial energy metabolism pathways.

Methods and results: In this study, we demonstrated that macrophage cholesterol efflux is regulated by mitochondrial ATP production, and that miR-33 controls a network of genes that synchronize mitochondrial function. Inhibition of mitochondrial ATP synthase markedly reduces macrophage cholesterol efflux capacity, and anti-miR33 required fully functional mitochondria to enhance ABCA1-mediated cholesterol efflux. Specifically, anti-miR33 derepressed the novel target genes PGC-1α, PDK4, and SLC25A25 and boosted mitochondrial respiration and production of ATP. Treatment of atherosclerotic Apoe(-/-) mice with anti-miR33 oligonucleotides reduced aortic sinus lesion area compared with controls, despite no changes in high-density lipoprotein cholesterol or other circulating lipids. Expression of miR-33a/b was markedly increased in human carotid atherosclerotic plaques compared with normal arteries, and there was a concomitant decrease in mitochondrial regulatory genes PGC-1α, SLC25A25, NRF1, and TFAM, suggesting these genes are associated with advanced atherosclerosis in humans.

Conclusions: This study demonstrates that anti-miR33 therapy derepresses genes that enhance mitochondrial respiration and ATP production, which in conjunction with increased ABCA1 expression, works to promote macrophage cholesterol efflux and reduce atherosclerosis.

Keywords: atherosclerosis; cholesterol; macrophages; microRNA-33, mouse; mitochondria.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Adenosine Triphosphate / biosynthesis*
  • Amino Acid Transport Systems, Acidic / biosynthesis
  • Amino Acid Transport Systems, Acidic / genetics
  • Animals
  • Apolipoproteins E / deficiency
  • Atherosclerosis / genetics
  • Atherosclerosis / metabolism*
  • Atherosclerosis / therapy
  • Base Sequence
  • Calcium-Binding Proteins / biosynthesis
  • Calcium-Binding Proteins / genetics
  • Cell Line
  • Cholesterol / metabolism*
  • Gene Expression Regulation / drug effects
  • Genetic Therapy
  • HEK293 Cells
  • Humans
  • Macrophages / metabolism*
  • Macrophages, Peritoneal / metabolism*
  • Mice
  • Mice, Inbred C57BL
  • MicroRNAs / antagonists & inhibitors*
  • MicroRNAs / genetics
  • Mitochondria / metabolism*
  • Mitochondrial Membrane Transport Proteins
  • Oligonucleotides, Antisense / pharmacology
  • Oligonucleotides, Antisense / therapeutic use*
  • Protein Serine-Threonine Kinases / genetics
  • Sequence Alignment
  • Sequence Homology, Nucleic Acid
  • Transcription Factors / biosynthesis
  • Transcription Factors / genetics

Substances

  • Amino Acid Transport Systems, Acidic
  • Apolipoproteins E
  • Calcium-Binding Proteins
  • MicroRNAs
  • Mirn33 microRNA, mouse
  • Mitochondrial Membrane Transport Proteins
  • Oligonucleotides, Antisense
  • SLC25A25 protein, human
  • Transcription Factors
  • Adenosine Triphosphate
  • Cholesterol
  • Protein Serine-Threonine Kinases