Limiting Mrs2-dependent mitochondrial Mg2+ uptake induces metabolic programming in prolonged dietary stress

Travis R. Madaris; Manigandan Venkatesan; Soumya Maity; Miriam C. Stein; Neelanjan Vishnu; Mridula K. Venkateswaran; James G. Davis; Karthik Ramachandran; Sukanthathulse Uthayabalan; Cristel Allen; Ayodeji Osidele; Kristen Stanley; Nicholas P. Bigham; Terry M. Bakewell; Melanie Narkunan; Amy Le; Varsha Karanam; Kang Li; Aum Mhapankar; Luke Norton; Jean Ross; M. Imran Aslam; W. Brian Reeves; Brij B. Singh; Jeffrey Caplan; Justin J. Wilson; Peter B. Stathopulos; Joseph A. Baur; Muniswamy Madesh

doi:10.1016/j.celrep.2023.112155

Limiting Mrs2-dependent mitochondrial Mg²⁺ uptake induces metabolic programming in prolonged dietary stress

Travis R. Madaris, Manigandan Venkatesan, Soumya Maity, Miriam C. Stein, Neelanjan Vishnu, Mridula K. Venkateswaran, James G. Davis, Karthik Ramachandran, Sukanthathulse Uthayabalan, Cristel Allen, Ayodeji Osidele, Kristen Stanley, Nicholas P. Bigham, Terry M. Bakewell, Melanie Narkunan, Amy Le, Varsha Karanam, Kang Li, Aum Mhapankar, Luke NortonJean Ross, M. Imran Aslam, W. Brian Reeves, Brij B. Singh, Jeffrey Caplan, Justin J. Wilson, Peter B. Stathopulos, Joseph A. Baur, Muniswamy Madesh

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

16 Scopus citations

Abstract

The most abundant cellular divalent cations, Mg²⁺ (mM) and Ca²⁺ (nM-μM), antagonistically regulate divergent metabolic pathways with several orders of magnitude affinity preference, but the physiological significance of this competition remains elusive. In mice consuming a Western diet, genetic ablation of the mitochondrial Mg²⁺ channel Mrs2 prevents weight gain, enhances mitochondrial activity, decreases fat accumulation in the liver, and causes prominent browning of white adipose. Mrs2 deficiency restrains citrate efflux from the mitochondria, making it unavailable to support de novo lipogenesis. As citrate is an endogenous Mg²⁺ chelator, this may represent an adaptive response to a perceived deficit of the cation. Transcriptional profiling of liver and white adipose reveals higher expression of genes involved in glycolysis, β-oxidation, thermogenesis, and HIF-1α-targets, in Mrs2^−/− mice that are further enhanced under Western-diet-associated metabolic stress. Thus, lowering _mMg²⁺ promotes metabolism and dampens diet-induced obesity and metabolic syndrome.

Original language	English (US)
Article number	112155
Journal	Cell Reports
Volume	42
Issue number	3
DOIs	https://doi.org/10.1016/j.celrep.2023.112155
State	Published - Mar 28 2023

Keywords

CP: Metabolism
HCC
HIF1
MCU
Mrs2
NAFLD
Western diet
adipose expansion
adipose tissue
calcium channel
cardiometabolic disease
diabetes
energy imbalance
hepatocytes
liver
magnesium channel
metabolic disease
metabolic syndrome
mitochondrial dysfunction
obesity
whole-body metabolism

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.1016/j.celrep.2023.112155

Cite this

Madaris, T. R., Venkatesan, M., Maity, S., Stein, M. C., Vishnu, N., Venkateswaran, M. K., Davis, J. G., Ramachandran, K., Uthayabalan, S., Allen, C., Osidele, A., Stanley, K., Bigham, N. P., Bakewell, T. M., Narkunan, M., Le, A., Karanam, V., Li, K., Mhapankar, A., ... Madesh, M. (2023). Limiting Mrs2-dependent mitochondrial Mg²⁺ uptake induces metabolic programming in prolonged dietary stress. Cell Reports, 42(3), Article 112155. https://doi.org/10.1016/j.celrep.2023.112155

Madaris, TR, Venkatesan, M, Maity, S, Stein, MC, Vishnu, N, Venkateswaran, MK, Davis, JG, Ramachandran, K, Uthayabalan, S, Allen, C, Osidele, A, Stanley, K, Bigham, NP, Bakewell, TM, Narkunan, M, Le, A, Karanam, V, Li, K, Mhapankar, A, Norton, L, Ross, J, Aslam, MI, Reeves, WB , Singh, BB, Caplan, J, Wilson, JJ, Stathopulos, PB, Baur, JA & Madesh, M 2023, 'Limiting Mrs2-dependent mitochondrial Mg²⁺ uptake induces metabolic programming in prolonged dietary stress', Cell Reports, vol. 42, no. 3, 112155. https://doi.org/10.1016/j.celrep.2023.112155

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title = "Limiting Mrs2-dependent mitochondrial Mg2+ uptake induces metabolic programming in prolonged dietary stress",

abstract = "The most abundant cellular divalent cations, Mg2+ (mM) and Ca2+ (nM-μM), antagonistically regulate divergent metabolic pathways with several orders of magnitude affinity preference, but the physiological significance of this competition remains elusive. In mice consuming a Western diet, genetic ablation of the mitochondrial Mg2+ channel Mrs2 prevents weight gain, enhances mitochondrial activity, decreases fat accumulation in the liver, and causes prominent browning of white adipose. Mrs2 deficiency restrains citrate efflux from the mitochondria, making it unavailable to support de novo lipogenesis. As citrate is an endogenous Mg2+ chelator, this may represent an adaptive response to a perceived deficit of the cation. Transcriptional profiling of liver and white adipose reveals higher expression of genes involved in glycolysis, β-oxidation, thermogenesis, and HIF-1α-targets, in Mrs2−/− mice that are further enhanced under Western-diet-associated metabolic stress. Thus, lowering mMg2+ promotes metabolism and dampens diet-induced obesity and metabolic syndrome.",

keywords = "CP: Metabolism, HCC, HIF1, MCU, Mrs2, NAFLD, Western diet, adipose expansion, adipose tissue, calcium channel, cardiometabolic disease, diabetes, energy imbalance, hepatocytes, liver, magnesium channel, metabolic disease, metabolic syndrome, mitochondrial dysfunction, obesity, whole-body metabolism",

author = "Madaris, {Travis R.} and Manigandan Venkatesan and Soumya Maity and Stein, {Miriam C.} and Neelanjan Vishnu and Venkateswaran, {Mridula K.} and Davis, {James G.} and Karthik Ramachandran and Sukanthathulse Uthayabalan and Cristel Allen and Ayodeji Osidele and Kristen Stanley and Bigham, {Nicholas P.} and Bakewell, {Terry M.} and Melanie Narkunan and Amy Le and Varsha Karanam and Kang Li and Aum Mhapankar and Luke Norton and Jean Ross and Aslam, {M. Imran} and Reeves, {W. Brian} and Singh, {Brij B.} and Jeffrey Caplan and Wilson, {Justin J.} and Stathopulos, {Peter B.} and Baur, {Joseph A.} and Muniswamy Madesh",

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doi = "10.1016/j.celrep.2023.112155",

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T1 - Limiting Mrs2-dependent mitochondrial Mg2+ uptake induces metabolic programming in prolonged dietary stress

AU - Madaris, Travis R.

AU - Venkatesan, Manigandan

AU - Maity, Soumya

AU - Stein, Miriam C.

AU - Vishnu, Neelanjan

AU - Venkateswaran, Mridula K.

AU - Davis, James G.

AU - Ramachandran, Karthik

AU - Uthayabalan, Sukanthathulse

AU - Allen, Cristel

AU - Osidele, Ayodeji

AU - Stanley, Kristen

AU - Bigham, Nicholas P.

AU - Bakewell, Terry M.

AU - Narkunan, Melanie

AU - Le, Amy

AU - Karanam, Varsha

AU - Li, Kang

AU - Mhapankar, Aum

AU - Norton, Luke

AU - Ross, Jean

AU - Aslam, M. Imran

AU - Reeves, W. Brian

AU - Singh, Brij B.

AU - Caplan, Jeffrey

AU - Wilson, Justin J.

AU - Stathopulos, Peter B.

AU - Baur, Joseph A.

AU - Madesh, Muniswamy

PY - 2023/3/28

Y1 - 2023/3/28

N2 - The most abundant cellular divalent cations, Mg2+ (mM) and Ca2+ (nM-μM), antagonistically regulate divergent metabolic pathways with several orders of magnitude affinity preference, but the physiological significance of this competition remains elusive. In mice consuming a Western diet, genetic ablation of the mitochondrial Mg2+ channel Mrs2 prevents weight gain, enhances mitochondrial activity, decreases fat accumulation in the liver, and causes prominent browning of white adipose. Mrs2 deficiency restrains citrate efflux from the mitochondria, making it unavailable to support de novo lipogenesis. As citrate is an endogenous Mg2+ chelator, this may represent an adaptive response to a perceived deficit of the cation. Transcriptional profiling of liver and white adipose reveals higher expression of genes involved in glycolysis, β-oxidation, thermogenesis, and HIF-1α-targets, in Mrs2−/− mice that are further enhanced under Western-diet-associated metabolic stress. Thus, lowering mMg2+ promotes metabolism and dampens diet-induced obesity and metabolic syndrome.

AB - The most abundant cellular divalent cations, Mg2+ (mM) and Ca2+ (nM-μM), antagonistically regulate divergent metabolic pathways with several orders of magnitude affinity preference, but the physiological significance of this competition remains elusive. In mice consuming a Western diet, genetic ablation of the mitochondrial Mg2+ channel Mrs2 prevents weight gain, enhances mitochondrial activity, decreases fat accumulation in the liver, and causes prominent browning of white adipose. Mrs2 deficiency restrains citrate efflux from the mitochondria, making it unavailable to support de novo lipogenesis. As citrate is an endogenous Mg2+ chelator, this may represent an adaptive response to a perceived deficit of the cation. Transcriptional profiling of liver and white adipose reveals higher expression of genes involved in glycolysis, β-oxidation, thermogenesis, and HIF-1α-targets, in Mrs2−/− mice that are further enhanced under Western-diet-associated metabolic stress. Thus, lowering mMg2+ promotes metabolism and dampens diet-induced obesity and metabolic syndrome.

KW - CP: Metabolism

KW - HCC

KW - HIF1

KW - MCU

KW - Mrs2

KW - NAFLD

KW - Western diet

KW - adipose expansion

KW - adipose tissue

KW - calcium channel

KW - cardiometabolic disease

KW - diabetes

KW - energy imbalance

KW - hepatocytes

KW - liver

KW - magnesium channel

KW - metabolic disease

KW - metabolic syndrome

KW - mitochondrial dysfunction

KW - obesity

KW - whole-body metabolism

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