ADH5-mediated NO bioactivity maintains metabolic homeostasis in brown adipose tissue

Sara C. Sebag; Zeyuan Zhang; Qingwen Qian; Mark Li; Zhiyong Zhu; Mikako Harata; Wenxian Li; Leonid V. Zingman; Limin Liu; Vitor A. Lira; Matthew J. Potthoff; Alexander Bartelt; Ling Yang

doi:10.1016/j.celrep.2021.110003

ADH5-mediated NO bioactivity maintains metabolic homeostasis in brown adipose tissue

Sara C. Sebag
, Zeyuan Zhang
, Qingwen Qian
, Mark Li
, Zhiyong Zhu
, Mikako Harata
, Wenxian Li
, Leonid V. Zingman
, Limin Liu
, Vitor A. Lira
, Matthew J. Potthoff
, Alexander Bartelt
, Ling Yang

Chair of Translational Nutritional Medicine

University of Iowa Carver College of Medicine
University of Iowa Carver College of Medicine
University of California San Francisco
College of Liberal Arts and Sciences
Ludwig-Maximilians-Universität München
Helmholtz Zentrum München German Research Center for Environmental Health
Harvard T.H. Chan School of Public Health

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

19 Scopus citations

Abstract

Brown adipose tissue (BAT) thermogenic activity is tightly regulated by cellular redox status, but the underlying molecular mechanisms are incompletely understood. Protein S-nitrosylation, the nitric-oxide-mediated cysteine thiol protein modification, plays important roles in cellular redox regulation. Here we show that diet-induced obesity (DIO) and acute cold exposure elevate BAT protein S-nitrosylation, including UCP1. This thermogenic-induced nitric oxide bioactivity is regulated by S-nitrosoglutathione reductase (GSNOR; alcohol dehydrogenase 5 [ADH5]), a denitrosylase that balances the intracellular nitroso-redox status. Loss of ADH5 in BAT impairs cold-induced UCP1-dependent thermogenesis and worsens obesity-associated metabolic dysfunction. Mechanistically, we demonstrate that Adh5 expression is induced by the transcription factor heat shock factor 1 (HSF1), and administration of an HSF1 activator to BAT of DIO mice increases Adh5 expression and significantly improves UCP1-mediated respiration. Together, these data indicate that ADH5 controls BAT nitroso-redox homeostasis to regulate adipose thermogenesis, which may be therapeutically targeted to improve metabolic health.

Original language	English
Article number	110003
Journal	Cell Reports
Volume	37
Issue number	7
DOIs	https://doi.org/10.1016/j.celrep.2021.110003
State	Published - 16 Nov 2021

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

ADH5
BAT
HSF1
alcohol dehydrogenase 5
brown adipose tissue
heat shock factor 1
nitrosative stress
obesity

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10.1016/j.celrep.2021.110003

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title = "ADH5-mediated NO bioactivity maintains metabolic homeostasis in brown adipose tissue",

abstract = "Brown adipose tissue (BAT) thermogenic activity is tightly regulated by cellular redox status, but the underlying molecular mechanisms are incompletely understood. Protein S-nitrosylation, the nitric-oxide-mediated cysteine thiol protein modification, plays important roles in cellular redox regulation. Here we show that diet-induced obesity (DIO) and acute cold exposure elevate BAT protein S-nitrosylation, including UCP1. This thermogenic-induced nitric oxide bioactivity is regulated by S-nitrosoglutathione reductase (GSNOR; alcohol dehydrogenase 5 [ADH5]), a denitrosylase that balances the intracellular nitroso-redox status. Loss of ADH5 in BAT impairs cold-induced UCP1-dependent thermogenesis and worsens obesity-associated metabolic dysfunction. Mechanistically, we demonstrate that Adh5 expression is induced by the transcription factor heat shock factor 1 (HSF1), and administration of an HSF1 activator to BAT of DIO mice increases Adh5 expression and significantly improves UCP1-mediated respiration. Together, these data indicate that ADH5 controls BAT nitroso-redox homeostasis to regulate adipose thermogenesis, which may be therapeutically targeted to improve metabolic health.",

keywords = "ADH5, BAT, HSF1, alcohol dehydrogenase 5, brown adipose tissue, heat shock factor 1, nitrosative stress, obesity",

author = "Sebag, \{Sara C.\} and Zeyuan Zhang and Qingwen Qian and Mark Li and Zhiyong Zhu and Mikako Harata and Wenxian Li and Zingman, \{Leonid V.\} and Limin Liu and Lira, \{Vitor A.\} and Potthoff, \{Matthew J.\} and Alexander Bartelt and Ling Yang",

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AU - Sebag, Sara C.

AU - Zhang, Zeyuan

AU - Qian, Qingwen

AU - Li, Mark

AU - Zhu, Zhiyong

AU - Harata, Mikako

AU - Li, Wenxian

AU - Zingman, Leonid V.

AU - Liu, Limin

AU - Lira, Vitor A.

AU - Potthoff, Matthew J.

AU - Bartelt, Alexander

AU - Yang, Ling

PY - 2021/11/16

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N2 - Brown adipose tissue (BAT) thermogenic activity is tightly regulated by cellular redox status, but the underlying molecular mechanisms are incompletely understood. Protein S-nitrosylation, the nitric-oxide-mediated cysteine thiol protein modification, plays important roles in cellular redox regulation. Here we show that diet-induced obesity (DIO) and acute cold exposure elevate BAT protein S-nitrosylation, including UCP1. This thermogenic-induced nitric oxide bioactivity is regulated by S-nitrosoglutathione reductase (GSNOR; alcohol dehydrogenase 5 [ADH5]), a denitrosylase that balances the intracellular nitroso-redox status. Loss of ADH5 in BAT impairs cold-induced UCP1-dependent thermogenesis and worsens obesity-associated metabolic dysfunction. Mechanistically, we demonstrate that Adh5 expression is induced by the transcription factor heat shock factor 1 (HSF1), and administration of an HSF1 activator to BAT of DIO mice increases Adh5 expression and significantly improves UCP1-mediated respiration. Together, these data indicate that ADH5 controls BAT nitroso-redox homeostasis to regulate adipose thermogenesis, which may be therapeutically targeted to improve metabolic health.

AB - Brown adipose tissue (BAT) thermogenic activity is tightly regulated by cellular redox status, but the underlying molecular mechanisms are incompletely understood. Protein S-nitrosylation, the nitric-oxide-mediated cysteine thiol protein modification, plays important roles in cellular redox regulation. Here we show that diet-induced obesity (DIO) and acute cold exposure elevate BAT protein S-nitrosylation, including UCP1. This thermogenic-induced nitric oxide bioactivity is regulated by S-nitrosoglutathione reductase (GSNOR; alcohol dehydrogenase 5 [ADH5]), a denitrosylase that balances the intracellular nitroso-redox status. Loss of ADH5 in BAT impairs cold-induced UCP1-dependent thermogenesis and worsens obesity-associated metabolic dysfunction. Mechanistically, we demonstrate that Adh5 expression is induced by the transcription factor heat shock factor 1 (HSF1), and administration of an HSF1 activator to BAT of DIO mice increases Adh5 expression and significantly improves UCP1-mediated respiration. Together, these data indicate that ADH5 controls BAT nitroso-redox homeostasis to regulate adipose thermogenesis, which may be therapeutically targeted to improve metabolic health.

KW - ADH5

KW - BAT

KW - HSF1

KW - alcohol dehydrogenase 5

KW - brown adipose tissue

KW - heat shock factor 1

KW - nitrosative stress

KW - obesity

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ADH5-mediated NO bioactivity maintains metabolic homeostasis in brown adipose tissue

Abstract

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Keywords

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