Mitofusin-2 Determines Mitochondrial Network Architecture and Mitochondrial Metabolism

Bach, D; Pich, Sara; Soriano, Francesc X.; Véga, Nathalie; Baumgartner, Bernhard; Oriola, Josep; Daugaard, Jens R.; Lloberas, Jorge; Camps, Marta; Zierath, Juleen R.; Rabasa‐Lhoret, Rémi; Wallberg-Henriksson, Harriet; Laville, Martine; Palacı́n, Manuel; Vidal, Hubert; Rivera, Francisca; Brand, Martin D.; Zorzano, António

doi:10.1074/jbc.m212754200

Cited by 748 publications

(743 citation statements)

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“…Mfn2 can also interact directly with Ced9 or BclxL in HEK293 cells suggesting a mechanism for crosstalk with antiapoptotic Bcl family proteins [71]. Mfn2 has been shown to modulate metabolism [104,105] and cell cycle [106]. We therefore suggest that Mfn2, unlike Mfn1, may be able to provide additional protection against neuronal apoptosis through mitochondrial fusion independent mechanism, such as metabolic and cell cycle control (Fig.…”

Section: The Role Of Mitochondrial Fusion In Cell Death: Mfn1 and Mfnmentioning

confidence: 89%

“…In the following section we will discuss the mitochondrial fusion independent role of Mfn2 in metabolism, cell cycle control and apoptosis. Studies in diabetic model systems have indicated that the reduction of Mfn2 leads to an inhibition of glucose oxidation and cell respiration, which is linked to obesity in both rat and human [104]. Mfn2 control of metabolism is not dependent on mitochondrial fusion, since expression of a truncated form of Mfn2 that is localized in cytoplasm can still increase mitochondrial respiration.…”

Section: The Role Of Mitochondrial Fusion In Cell Death: Mfn1 and Mfnmentioning

confidence: 99%

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Mitochondrial dynamics in the regulation of neuronal cell death

2007

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Mitochondria undergo continuous fission and fusion events in physiological situations. Fragmentation of mitochondria during cell death has been shown to play a key role in cell death progression, including release of the mitochondrial apoptotic proteins. Ultrastructural changes in mitochondria, such as cristae remodeling, is also involved in cell death initiation. Here, we emphasize the important role of mitochondrial fission/fusion machinery in neuronal cell death. Unlike many other cell types such as immortalized cell lines, neurons are distinct morphologically and functionally. We will discuss how this uniqueness presents special challenges in the cellular response to neurotoxic stresses, and how this affects the mitochondrial dynamics in the regulation of cell death in neurons.

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Section: The Role Of Mitochondrial Fusion In Cell Death: Mfn1 and Mfnmentioning

confidence: 89%

Section: The Role Of Mitochondrial Fusion In Cell Death: Mfn1 and Mfnmentioning

confidence: 99%

Mitochondrial dynamics in the regulation of neuronal cell death

2007

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“…However, while this investigation found no changes in apoptosis in DOX‐treated HL‐1 cardiomyocytes in the presence of Nox2 or Mfn2 knockdown, it is possible that efficacy of transfection may have influenced the measured endpoint. Indeed, highly oxidative tissues such as the heart require constant energy production, and as mitochondria are the powerhouse of the cardiomyocyte comprising a large proportion of cytoplasmic volume, it is possible that there is such a high level of Mfn2 expression in HL‐1 cardiomyocytes that the observed effects of Mfn2 siRNA on cell apoptosis may have underestimated the involvement of Mfn2 (Bach et al, 2003; Papanicolaou et al, 2011). Indeed, when a higher level of knockdown was achieved, a lack of Mfn2 corresponded with reduction of caspase 3/7 activity, assessed by both DEVD and PARP‐1 cleavage.…”

Section: Discussionmentioning

confidence: 99%

Signalling mechanisms underlying doxorubicin and Nox2 NADPH oxidase‐induced cardiomyopathy: involvement of mitofusin‐2

McLaughlin

Zhao

O’Neill

et al. 2017

British J Pharmacology

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Background and PurposeThe anthracycline doxorubicin (DOX), although successful as a first‐line cancer treatment, induces cardiotoxicity linked with increased production of myocardial ROS, with Nox2 NADPH oxidase‐derived superoxide reported to play a key role. The aim of this study was to identify novel mechanisms underlying development of cardiac remodelling/dysfunction further to DOX‐stimulated Nox2 activation.Experimental ApproachNox2−/− and wild‐type (WT) littermate mice were administered DOX (12 mg·kg−1 over 3 weeks) prior to study at 4 weeks. Detailed mechanisms were investigated in murine HL‐1 cardiomyocytes, employing a robust model of oxidative stress, gene silencing and pharmacological tools.Key ResultsDOX‐induced cardiac dysfunction, cardiomyocyte remodelling, superoxide production and apoptosis in WT mice were attenuated in Nox2−/− mice. Transcriptional analysis of left ventricular tissue identified 152 differentially regulated genes (using adjusted P < 0.1) in DOX‐treated Nox2−/− versus WT mice, and network analysis highlighted ‘Cell death and survival’ as the biological function most significant to the dataset. The mitochondrial membrane protein, mitofusin‐2 (Mfn2), appeared as a strong candidate, with increased expression (1.5‐fold), confirmed by qPCR (1.3‐fold), matching clear published evidence of promotion of cardiomyocyte cell death. In HL‐1 cardiomyocytes, targeted siRNA knockdown of Nox2 decreased Mfn2 protein expression, but not vice versa. While inhibition of Nox2 activity along with DOX treatment attenuated its apoptotic and cytotoxic effects, reduced apoptosis after Mfn2 silencing reflected a sustained cytotoxic response and reduced cell viability.Conclusions and ImplicationsDOX‐induced and Nox2‐mediated up‐regulation of Mfn2, rather than contributing to cardiomyocyte dysfunction through apoptotic pathways, appears to promote a protective mechanism.Linked ArticlesThis article is part of a themed section on New Insights into Cardiotoxicity Caused by Chemotherapeutic Agents. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v174.21/issuetoc

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“…Mfn2 expression is ubiquitous in mammalian tissues, albeit it finds its highest expression levels in tissues enriched in mitochondria, such as heart and the brown adipose tissue (BAT) (Bach et al , 2003). Recently, the BAT has gained significant attraction after its identification and localization in humans (for review, see Peirce et al , 2014).…”

Section: Introductionmentioning

confidence: 99%

Mfn2 is critical for brown adipose tissue thermogenic function

et al. 2017

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Mitochondrial fusion and fission events, collectively known as mitochondrial dynamics, act as quality control mechanisms to ensure mitochondrial function and fine‐tune cellular bioenergetics. Defective mitofusin 2 (Mfn2) expression and enhanced mitochondrial fission in skeletal muscle are hallmarks of insulin‐resistant states. Interestingly, Mfn2 is highly expressed in brown adipose tissue (BAT), yet its role remains unexplored. Using adipose‐specific Mfn2 knockout (Mfn2‐adKO) mice, we demonstrate that Mfn2, but not Mfn1, deficiency in BAT leads to a profound BAT dysfunction, associated with impaired respiratory capacity and a blunted response to adrenergic stimuli. Importantly, Mfn2 directly interacts with perilipin 1, facilitating the interaction between the mitochondria and the lipid droplet in response to adrenergic stimulation. Surprisingly, Mfn2‐adKO mice were protected from high‐fat diet‐induced insulin resistance and hepatic steatosis. Altogether, these results demonstrate that Mfn2 is a mediator of mitochondria to lipid droplet interactions, influencing lipolytic processes and whole‐body energy homeostasis.

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Mitofusin-2 Determines Mitochondrial Network Architecture and Mitochondrial Metabolism

Cited by 748 publications

References 51 publications

Mitochondrial dynamics in the regulation of neuronal cell death

Mitochondrial dynamics in the regulation of neuronal cell death

Signalling mechanisms underlying doxorubicin and Nox2 NADPH oxidase‐induced cardiomyopathy: involvement of mitofusin‐2

Mfn2 is critical for brown adipose tissue thermogenic function

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