Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling

Zhenqi Zhou; Timothy M. Moore; Brian G. Drew; Vicent Ribas; Jonathan Wanagat; Mete Civelek; Mayuko Segawa; Dane M. Wolf; Frode Norheim; Marcus M. Seldin; Alexander R. Strumwasser; Kate A. Whitney; Ellen Lester; Britany R. Reddish; Laurent Vergnes; Karen Reue; Prashant Rajbhandari; Peter Tontonoz; Jason Lee; Sushil K. Mahata; Sylvia C. Hewitt; Orian Shirihai; Craig Gastonbury; Kerrin S. Small; Markku Laakso; Jorgen Jensen; Sindre Lee; Christian A. Drevon; Kenneth S. Korach; Aldons J. Lusis; Andrea L. Hevener

doi:10.1126/SCITRANSLMED.AAX8096

Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling

Zhenqi Zhou, Timothy M. Moore, Brian G. Drew, Vicent Ribas, Jonathan Wanagat, Mete Civelek, Mayuko Segawa, Dane M. Wolf, Frode Norheim, Marcus M. Seldin, Alexander R. Strumwasser, Kate A. Whitney, Ellen Lester, Britany R. Reddish, Laurent Vergnes, Karen Reue, Prashant Rajbhandari, Peter Tontonoz, Jason Lee, Sushil K. MahataSylvia C. Hewitt, Orian Shirihai, Craig Gastonbury, Kerrin S. Small, Markku Laakso, Jorgen Jensen, Sindre Lee, Christian A. Drevon, Kenneth S. Korach, Aldons J. Lusis, Andrea L. Hevener

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

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Abstract

Obesity is heightened during aging, and although the estrogen receptor α (ERα) has been implicated in the prevention of obesity, its molecular actions in adipocytes remain inadequately understood. Here, we show that adipose tissue ESR1/Esr1 expression inversely associated with adiposity and positively associated with genes involved in mitochondrial metabolism and markers of metabolic health in 700 Finnish men and 100 strains of inbred mice from the UCLA Hybrid Mouse Diversity Panel. To determine the anti-obesity actions of ERα in fat, we selectively deleted Esr1 from white and brown adipocytes in mice. In white adipose tissue, Esr1 controlled oxidative metabolism by restraining the targeted elimination of mitochondria via the E3 ubiquitin ligase parkin. mtDNA content was elevated, and adipose tissue mass was reduced in adipose-selective parkin knockout mice. In brown fat centrally involved in body temperature maintenance, Esr1 was requisite for both mitochondrial remodeling by dynamin-related protein 1 (Drp1) and uncoupled respiration thermogenesis by uncoupled protein 1 (Ucp1). In both white and brown fat of female mice and adipocytes in culture, mitochondrial dysfunction in the context of Esr1 deletion was paralleled by a reduction in the expression of the mtDNA polymerase γ subunit Polg1. We identified Polg1 as an ERα target gene by showing that ERα binds the Polg1 promoter to control its expression in 3T3L1 adipocytes. These findings support strategies leveraging ERα action on mitochondrial function in adipocytes to combat obesity and metabolic dysfunction.

Original language	English
Article number	eaax8096
Journal	Science Translational Medicine
Volume	12
Issue number	555
DOIs	https://doi.org/10.1126/SCITRANSLMED.AAX8096
State	Published - 5 Aug 2020
Externally published	Yes

ASJC Scopus subject areas

Medicine (all)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1126/SCITRANSLMED.AAX8096

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Zhou, Z., Moore, T. M., Drew, B. G., Ribas, V., Wanagat, J., Civelek, M., Segawa, M., Wolf, D. M., Norheim, F., Seldin, M. M., Strumwasser, A. R., Whitney, K. A., Lester, E., Reddish, B. R., Vergnes, L., Reue, K., Rajbhandari, P., Tontonoz, P., Lee, J., ... Hevener, A. L. (2020). Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling. Science Translational Medicine, 12(555), Article eaax8096. https://doi.org/10.1126/SCITRANSLMED.AAX8096

@article{db8c20dc45f04277aaf4186bfda7c281,

title = "Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling",

abstract = "Obesity is heightened during aging, and although the estrogen receptor α (ERα) has been implicated in the prevention of obesity, its molecular actions in adipocytes remain inadequately understood. Here, we show that adipose tissue ESR1/Esr1 expression inversely associated with adiposity and positively associated with genes involved in mitochondrial metabolism and markers of metabolic health in 700 Finnish men and 100 strains of inbred mice from the UCLA Hybrid Mouse Diversity Panel. To determine the anti-obesity actions of ERα in fat, we selectively deleted Esr1 from white and brown adipocytes in mice. In white adipose tissue, Esr1 controlled oxidative metabolism by restraining the targeted elimination of mitochondria via the E3 ubiquitin ligase parkin. mtDNA content was elevated, and adipose tissue mass was reduced in adipose-selective parkin knockout mice. In brown fat centrally involved in body temperature maintenance, Esr1 was requisite for both mitochondrial remodeling by dynamin-related protein 1 (Drp1) and uncoupled respiration thermogenesis by uncoupled protein 1 (Ucp1). In both white and brown fat of female mice and adipocytes in culture, mitochondrial dysfunction in the context of Esr1 deletion was paralleled by a reduction in the expression of the mtDNA polymerase γ subunit Polg1. We identified Polg1 as an ERα target gene by showing that ERα binds the Polg1 promoter to control its expression in 3T3L1 adipocytes. These findings support strategies leveraging ERα action on mitochondrial function in adipocytes to combat obesity and metabolic dysfunction.",

author = "Zhenqi Zhou and Moore, {Timothy M.} and Drew, {Brian G.} and Vicent Ribas and Jonathan Wanagat and Mete Civelek and Mayuko Segawa and Wolf, {Dane M.} and Frode Norheim and Seldin, {Marcus M.} and Strumwasser, {Alexander R.} and Whitney, {Kate A.} and Ellen Lester and Reddish, {Britany R.} and Laurent Vergnes and Karen Reue and Prashant Rajbhandari and Peter Tontonoz and Jason Lee and Mahata, {Sushil K.} and Hewitt, {Sylvia C.} and Orian Shirihai and Craig Gastonbury and Small, {Kerrin S.} and Markku Laakso and Jorgen Jensen and Sindre Lee and Drevon, {Christian A.} and Korach, {Kenneth S.} and Lusis, {Aldons J.} and Hevener, {Andrea L.}",

note = "Funding Information: This research was supported by funding to A.L.H. from the UCLA Department of Medicine, the Iris Cantor-UCLA Women{\textquoteright}s Health Center Research Foundation and UCLA CTSI (ULTR000124), the UCLA Claude D. Pepper Older Americans Independence Center, and the NIH (DK109724, P30DK063491, and NURSA NDSP under parent award U24DK097748). Z.Z. was supported by the UCLA Claude Pepper Older Americans Independence Center funded by the National Institute of Aging (5P30AG028748), the NIH/ NCATS UCLA CTSI Grant (UL1TR000124), and the UCLA Center for Duchenne Muscular Dystrophy-NIH NIAMS (U54 AR052646) Wellstone Center of Excellence Training. T.M.M. was supported by a Kirschstein-NRSA predoctoral fellowship (F31DK108657), a Carl V. Gisolfi Memorial Research grant from the American College of Sports Medicine, and a predoctoral graduate student award from the Dornsife College at the University of Southern California. S.K.M. was supported by a grant from the Department of Veterans Affairs (I01BX000323). K.S.K. was supported by the NIEHS Division of Intramural Research 1ZIAES070065. A.J.L. was supported by NIH grants HL28481 and HL30568. K.R., A.J.L., and A.L.H. are collaboratively supported by an NIH SCORE on Sex Differences and Women{\textquoteright}s Health (U54DK120342). Publisher Copyright: Copyright {\textcopyright} 2020 The Authors, some rights reserved.",

year = "2020",

month = aug,

day = "5",

doi = "10.1126/SCITRANSLMED.AAX8096",

language = "English",

volume = "12",

journal = "Science Translational Medicine",

issn = "1946-6234",

publisher = "American Association for the Advancement of Science",

number = "555",

}

Zhou, Z, Moore, TM, Drew, BG, Ribas, V, Wanagat, J, Civelek, M, Segawa, M, Wolf, DM, Norheim, F, Seldin, MM, Strumwasser, AR, Whitney, KA, Lester, E, Reddish, BR, Vergnes, L, Reue, K, Rajbhandari, P, Tontonoz, P, Lee, J, Mahata, SK, Hewitt, SC, Shirihai, O, Gastonbury, C, Small, KS, Laakso, M, Jensen, J, Lee, S, Drevon, CA, Korach, KS, Lusis, AJ & Hevener, AL 2020, 'Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling', Science Translational Medicine, vol. 12, no. 555, eaax8096. https://doi.org/10.1126/SCITRANSLMED.AAX8096

TY - JOUR

T1 - Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling

AU - Zhou, Zhenqi

AU - Moore, Timothy M.

AU - Drew, Brian G.

AU - Ribas, Vicent

AU - Wanagat, Jonathan

AU - Civelek, Mete

AU - Segawa, Mayuko

AU - Wolf, Dane M.

AU - Norheim, Frode

AU - Seldin, Marcus M.

AU - Strumwasser, Alexander R.

AU - Whitney, Kate A.

AU - Lester, Ellen

AU - Reddish, Britany R.

AU - Vergnes, Laurent

AU - Reue, Karen

AU - Rajbhandari, Prashant

AU - Tontonoz, Peter

AU - Lee, Jason

AU - Mahata, Sushil K.

AU - Hewitt, Sylvia C.

AU - Shirihai, Orian

AU - Gastonbury, Craig

AU - Small, Kerrin S.

AU - Laakso, Markku

AU - Jensen, Jorgen

AU - Lee, Sindre

AU - Drevon, Christian A.

AU - Korach, Kenneth S.

AU - Lusis, Aldons J.

AU - Hevener, Andrea L.

N1 - Funding Information: This research was supported by funding to A.L.H. from the UCLA Department of Medicine, the Iris Cantor-UCLA Women’s Health Center Research Foundation and UCLA CTSI (ULTR000124), the UCLA Claude D. Pepper Older Americans Independence Center, and the NIH (DK109724, P30DK063491, and NURSA NDSP under parent award U24DK097748). Z.Z. was supported by the UCLA Claude Pepper Older Americans Independence Center funded by the National Institute of Aging (5P30AG028748), the NIH/ NCATS UCLA CTSI Grant (UL1TR000124), and the UCLA Center for Duchenne Muscular Dystrophy-NIH NIAMS (U54 AR052646) Wellstone Center of Excellence Training. T.M.M. was supported by a Kirschstein-NRSA predoctoral fellowship (F31DK108657), a Carl V. Gisolfi Memorial Research grant from the American College of Sports Medicine, and a predoctoral graduate student award from the Dornsife College at the University of Southern California. S.K.M. was supported by a grant from the Department of Veterans Affairs (I01BX000323). K.S.K. was supported by the NIEHS Division of Intramural Research 1ZIAES070065. A.J.L. was supported by NIH grants HL28481 and HL30568. K.R., A.J.L., and A.L.H. are collaboratively supported by an NIH SCORE on Sex Differences and Women’s Health (U54DK120342). Publisher Copyright: Copyright © 2020 The Authors, some rights reserved.

PY - 2020/8/5

Y1 - 2020/8/5

N2 - Obesity is heightened during aging, and although the estrogen receptor α (ERα) has been implicated in the prevention of obesity, its molecular actions in adipocytes remain inadequately understood. Here, we show that adipose tissue ESR1/Esr1 expression inversely associated with adiposity and positively associated with genes involved in mitochondrial metabolism and markers of metabolic health in 700 Finnish men and 100 strains of inbred mice from the UCLA Hybrid Mouse Diversity Panel. To determine the anti-obesity actions of ERα in fat, we selectively deleted Esr1 from white and brown adipocytes in mice. In white adipose tissue, Esr1 controlled oxidative metabolism by restraining the targeted elimination of mitochondria via the E3 ubiquitin ligase parkin. mtDNA content was elevated, and adipose tissue mass was reduced in adipose-selective parkin knockout mice. In brown fat centrally involved in body temperature maintenance, Esr1 was requisite for both mitochondrial remodeling by dynamin-related protein 1 (Drp1) and uncoupled respiration thermogenesis by uncoupled protein 1 (Ucp1). In both white and brown fat of female mice and adipocytes in culture, mitochondrial dysfunction in the context of Esr1 deletion was paralleled by a reduction in the expression of the mtDNA polymerase γ subunit Polg1. We identified Polg1 as an ERα target gene by showing that ERα binds the Polg1 promoter to control its expression in 3T3L1 adipocytes. These findings support strategies leveraging ERα action on mitochondrial function in adipocytes to combat obesity and metabolic dysfunction.

AB - Obesity is heightened during aging, and although the estrogen receptor α (ERα) has been implicated in the prevention of obesity, its molecular actions in adipocytes remain inadequately understood. Here, we show that adipose tissue ESR1/Esr1 expression inversely associated with adiposity and positively associated with genes involved in mitochondrial metabolism and markers of metabolic health in 700 Finnish men and 100 strains of inbred mice from the UCLA Hybrid Mouse Diversity Panel. To determine the anti-obesity actions of ERα in fat, we selectively deleted Esr1 from white and brown adipocytes in mice. In white adipose tissue, Esr1 controlled oxidative metabolism by restraining the targeted elimination of mitochondria via the E3 ubiquitin ligase parkin. mtDNA content was elevated, and adipose tissue mass was reduced in adipose-selective parkin knockout mice. In brown fat centrally involved in body temperature maintenance, Esr1 was requisite for both mitochondrial remodeling by dynamin-related protein 1 (Drp1) and uncoupled respiration thermogenesis by uncoupled protein 1 (Ucp1). In both white and brown fat of female mice and adipocytes in culture, mitochondrial dysfunction in the context of Esr1 deletion was paralleled by a reduction in the expression of the mtDNA polymerase γ subunit Polg1. We identified Polg1 as an ERα target gene by showing that ERα binds the Polg1 promoter to control its expression in 3T3L1 adipocytes. These findings support strategies leveraging ERα action on mitochondrial function in adipocytes to combat obesity and metabolic dysfunction.

UR - http://www.scopus.com/inward/record.url?scp=85089171487&partnerID=8YFLogxK

U2 - 10.1126/SCITRANSLMED.AAX8096

DO - 10.1126/SCITRANSLMED.AAX8096

M3 - Article

AN - SCOPUS:85089171487

SN - 1946-6234

VL - 12

JO - Science Translational Medicine

JF - Science Translational Medicine

IS - 555

M1 - eaax8096

ER -

Estrogen receptor α controls metabolism in white and brown adipocytes by regulating Polg1 and mitochondrial remodeling

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