Reducing the mitochondrial oxidative burden alleviates lipid-induced muscle insulin resistance in humans

Matteo Fiorenza; Johan Onslev; Carlos Henríquez-Olguín; Kaspar W. Persson; Sofie A. Hesselager; Thomas E. Jensen; Jørgen F.P. Wojtaszewski; Morten Hostrup; Jens Bangsbo

doi:10.1126/sciadv.adq4461

Reducing the mitochondrial oxidative burden alleviates lipid-induced muscle insulin resistance in humans

Matteo Fiorenza^*, Johan Onslev, Carlos Henríquez-Olguín, Kaspar W. Persson, Sofie A. Hesselager, Thomas E. Jensen, Jørgen F.P. Wojtaszewski, Morten Hostrup, Jens Bangsbo

^*Corresponding author for this work

Research output: Contribution to journal › Journal article › Research › peer-review

3 Citations (Scopus)

8 Downloads (Pure)

Abstract

Preclinical models suggest mitochondria-derived oxidative stress as an underlying cause of insulin resistance. However, it remains unknown whether this pathophysiological mechanism is conserved in humans. Here, we used an invasive in vivo mechanistic approach to interrogate muscle insulin action while selectively manipulating the mitochondrial redox state in humans. To this end, we conducted insulin clamp studies combining intravenous infusion of a lipid overload with intake of a mitochondria-targeted antioxidant (mitoquinone). Under lipid overload, selective modulation of mitochondrial redox state by mitoquinone enhanced insulin-stimulated glucose uptake in skeletal muscle. Mechanistically, mitoquinone did not affect canonical insulin signaling but augmented insulin-stimulated glucose transporter type 4 (GLUT4) translocation while reducing the mitochondrial oxidative burden under lipid oversupply. Complementary ex vivo studies in human muscle fibers exposed to high intracellular lipid levels revealed that mitoquinone improves features of mitochondrial bioenergetics, including diminished mitochondrial H2O2 emission. These findings provide translational and mechanistic evidence implicating mitochondrial oxidants in the development of lipid-induced muscle insulin resistance in humans.

Original language	English
Article number	eadq4461
Journal	Science Advances
Volume	10
Issue number	44
Number of pages	20
ISSN	2375-2548
DOIs	https://doi.org/10.1126/sciadv.adq4461
Publication status	Published - 2024

Access to Document

10.1126/sciadv.adq4461Licence: CC BY-NC

FulltextFinal published version, 3.51 MBLicence: CC BY-NC

Cite this

@article{4fa5470c7eef43d981a37e2405833fda,

title = "Reducing the mitochondrial oxidative burden alleviates lipid-induced muscle insulin resistance in humans",

abstract = "Preclinical models suggest mitochondria-derived oxidative stress as an underlying cause of insulin resistance. However, it remains unknown whether this pathophysiological mechanism is conserved in humans. Here, we used an invasive in vivo mechanistic approach to interrogate muscle insulin action while selectively manipulating the mitochondrial redox state in humans. To this end, we conducted insulin clamp studies combining intravenous infusion of a lipid overload with intake of a mitochondria-targeted antioxidant (mitoquinone). Under lipid overload, selective modulation of mitochondrial redox state by mitoquinone enhanced insulin-stimulated glucose uptake in skeletal muscle. Mechanistically, mitoquinone did not affect canonical insulin signaling but augmented insulin-stimulated glucose transporter type 4 (GLUT4) translocation while reducing the mitochondrial oxidative burden under lipid oversupply. Complementary ex vivo studies in human muscle fibers exposed to high intracellular lipid levels revealed that mitoquinone improves features of mitochondrial bioenergetics, including diminished mitochondrial H2O2 emission. These findings provide translational and mechanistic evidence implicating mitochondrial oxidants in the development of lipid-induced muscle insulin resistance in humans.",

author = "Matteo Fiorenza and Johan Onslev and Carlos Henr{\'i}quez-Olgu{\'i}n and Persson, {Kaspar W.} and Hesselager, {Sofie A.} and Jensen, {Thomas E.} and Wojtaszewski, {J{\o}rgen F.P.} and Morten Hostrup and Jens Bangsbo",

year = "2024",

doi = "10.1126/sciadv.adq4461",

language = "English",

volume = "10",

journal = "Science Advances",

issn = "2375-2548",

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

number = "44",

}

TY - JOUR

T1 - Reducing the mitochondrial oxidative burden alleviates lipid-induced muscle insulin resistance in humans

AU - Fiorenza, Matteo

AU - Onslev, Johan

AU - Henríquez-Olguín, Carlos

AU - Persson, Kaspar W.

AU - Hesselager, Sofie A.

AU - Jensen, Thomas E.

AU - Wojtaszewski, Jørgen F.P.

AU - Hostrup, Morten

AU - Bangsbo, Jens

PY - 2024

Y1 - 2024

N2 - Preclinical models suggest mitochondria-derived oxidative stress as an underlying cause of insulin resistance. However, it remains unknown whether this pathophysiological mechanism is conserved in humans. Here, we used an invasive in vivo mechanistic approach to interrogate muscle insulin action while selectively manipulating the mitochondrial redox state in humans. To this end, we conducted insulin clamp studies combining intravenous infusion of a lipid overload with intake of a mitochondria-targeted antioxidant (mitoquinone). Under lipid overload, selective modulation of mitochondrial redox state by mitoquinone enhanced insulin-stimulated glucose uptake in skeletal muscle. Mechanistically, mitoquinone did not affect canonical insulin signaling but augmented insulin-stimulated glucose transporter type 4 (GLUT4) translocation while reducing the mitochondrial oxidative burden under lipid oversupply. Complementary ex vivo studies in human muscle fibers exposed to high intracellular lipid levels revealed that mitoquinone improves features of mitochondrial bioenergetics, including diminished mitochondrial H2O2 emission. These findings provide translational and mechanistic evidence implicating mitochondrial oxidants in the development of lipid-induced muscle insulin resistance in humans.

AB - Preclinical models suggest mitochondria-derived oxidative stress as an underlying cause of insulin resistance. However, it remains unknown whether this pathophysiological mechanism is conserved in humans. Here, we used an invasive in vivo mechanistic approach to interrogate muscle insulin action while selectively manipulating the mitochondrial redox state in humans. To this end, we conducted insulin clamp studies combining intravenous infusion of a lipid overload with intake of a mitochondria-targeted antioxidant (mitoquinone). Under lipid overload, selective modulation of mitochondrial redox state by mitoquinone enhanced insulin-stimulated glucose uptake in skeletal muscle. Mechanistically, mitoquinone did not affect canonical insulin signaling but augmented insulin-stimulated glucose transporter type 4 (GLUT4) translocation while reducing the mitochondrial oxidative burden under lipid oversupply. Complementary ex vivo studies in human muscle fibers exposed to high intracellular lipid levels revealed that mitoquinone improves features of mitochondrial bioenergetics, including diminished mitochondrial H2O2 emission. These findings provide translational and mechanistic evidence implicating mitochondrial oxidants in the development of lipid-induced muscle insulin resistance in humans.

U2 - 10.1126/sciadv.adq4461

DO - 10.1126/sciadv.adq4461

M3 - Journal article

C2 - 39475607

AN - SCOPUS:85208163795

SN - 2375-2548

VL - 10

JO - Science Advances

JF - Science Advances

IS - 44

M1 - eadq4461

ER -