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

Denuja Karunakaran; A. Brianne Thrush; My Anh Nguyen; Laura Richards; Michele Geoffrion; Ragunath Singaravelu; Eleni Ramphos; Prakriti Shangari; Mireille Ouimet; John P. Pezacki; Kathryn J. Moore; Ljubica Perisic; Lars Maegdefessel; Ulf Hedin; Mary Ellen Harper; Katey J. Rayner

doi:10.1161/CIRCRESAHA.117.305624

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

Denuja Karunakaran, A. Brianne Thrush, My Anh Nguyen, Laura Richards, Michele Geoffrion, Ragunath Singaravelu, Eleni Ramphos, Prakriti Shangari, Mireille Ouimet, John P. Pezacki, Kathryn J. Moore, Ljubica Perisic, Lars Maegdefessel, Ulf Hedin, Mary Ellen Harper, Katey J. Rayner

Research output: Contribution to journal › Article › Research › peer-review

163 Citations (Scopus)

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.

Original language	English
Pages (from-to)	266-278
Number of pages	13
Journal	Circulation Research
Volume	117
Issue number	3
DOIs	https://doi.org/10.1161/CIRCRESAHA.117.305624
Publication status	Published - 17 Jul 2015
Externally published	Yes

Keywords

atherosclerosis
cholesterol
macrophages
microRNA-33, mouse
mitochondria

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10.1161/CIRCRESAHA.117.305624

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Karunakaran, D., Thrush, A. B., Nguyen, M. A., Richards, L., Geoffrion, M., Singaravelu, R., Ramphos, E., Shangari, P., Ouimet, M., Pezacki, J. P., Moore, K. J., Perisic, L., Maegdefessel, L., Hedin, U., Harper, M. E., & Rayner, K. J. (2015). Macrophage Mitochondrial Energy Status Regulates Cholesterol Efflux and Is Enhanced by Anti-miR33 in Atherosclerosis. Circulation Research, 117(3), 266-278. https://doi.org/10.1161/CIRCRESAHA.117.305624

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

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",

author = "Denuja Karunakaran and Thrush, {A. Brianne} and Nguyen, {My Anh} and Laura Richards and Michele Geoffrion and Ragunath Singaravelu and Eleni Ramphos and Prakriti Shangari and Mireille Ouimet and Pezacki, {John P.} and Moore, {Kathryn J.} and Ljubica Perisic and Lars Maegdefessel and Ulf Hedin and Harper, {Mary Ellen} and Rayner, {Katey J.}",

note = "Publisher Copyright: {\textcopyright} 2015 American Heart Association, Inc.",

year = "2015",

month = jul,

day = "17",

doi = "10.1161/CIRCRESAHA.117.305624",

language = "English",

volume = "117",

pages = "266--278",

journal = "Circulation Research",

issn = "0009-7330",

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Karunakaran, D, Thrush, AB, Nguyen, MA, Richards, L, Geoffrion, M, Singaravelu, R, Ramphos, E, Shangari, P, Ouimet, M, Pezacki, JP, Moore, KJ, Perisic, L, Maegdefessel, L, Hedin, U, Harper, ME & Rayner, KJ 2015, 'Macrophage Mitochondrial Energy Status Regulates Cholesterol Efflux and Is Enhanced by Anti-miR33 in Atherosclerosis', Circulation Research, vol. 117, no. 3, pp. 266-278. https://doi.org/10.1161/CIRCRESAHA.117.305624

TY - JOUR

T1 - Macrophage Mitochondrial Energy Status Regulates Cholesterol Efflux and Is Enhanced by Anti-miR33 in Atherosclerosis

AU - Karunakaran, Denuja

AU - Thrush, A. Brianne

AU - Nguyen, My Anh

AU - Richards, Laura

AU - Geoffrion, Michele

AU - Singaravelu, Ragunath

AU - Ramphos, Eleni

AU - Shangari, Prakriti

AU - Ouimet, Mireille

AU - Pezacki, John P.

AU - Moore, Kathryn J.

AU - Perisic, Ljubica

AU - Maegdefessel, Lars

AU - Hedin, Ulf

AU - Harper, Mary Ellen

AU - Rayner, Katey J.

PY - 2015/7/17

Y1 - 2015/7/17

N2 - 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.

AB - 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.

KW - atherosclerosis

KW - cholesterol

KW - macrophages

KW - microRNA-33, mouse

KW - mitochondria

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U2 - 10.1161/CIRCRESAHA.117.305624

DO - 10.1161/CIRCRESAHA.117.305624

M3 - Article

C2 - 26002865

AN - SCOPUS:84937554657

SN - 0009-7330

VL - 117

SP - 266

EP - 278

JO - Circulation Research

JF - Circulation Research

IS - 3

ER -

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

Abstract

Keywords

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