Activated Mitofusin 2 Signals Mitochondrial Fusion, Interferes with Bax Activation, and Reduces Susceptibility to Radical Induced Depolarization

Neuspiel, Margaret; Zunino, Rodolfo; Gangaraju, Sandhya; Rippstein, Peter; McBride, Heidi M.

doi:10.1074/jbc.m501599200

Cited by 280 publications

(238 citation statements)

References 55 publications

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“…This would suggest that Mfn1 plays a more essential role in mediating fusion than Mfn2 or they may regulate fusion signaled from different pathways. While both Mfn1 and Mfn2 are important for mitochondrial fusion, a hydrolysis deficient form of Mfn2 was shown to stimulate mitochondrial fusion in cultured cells, and protected cells from apoptosis induced by staurosporine [79], which indicated additional regulatory functions for Mfn2. These suggest that apart from the fusion role, Mfn2 may also have additional functions that may impact the survival of cells.…”

Section: Mitochondrial Fusion Proteinsmentioning

confidence: 95%

“…Fusion is thought to protect mitochondrial function by allowing rapid mixing of membranes, mitochondrial DNA and soluble contents that may be damaged by localized deficits of substrates as a result of cellular stress [35]. Recently, several studies indicated that during cell death mitochondrial fusion is inhibited and activation of the fusion machinery could slow down the rate of cell death [29,69,79]. There are, however, some very significant differences in the action of the fusion proteins in the regulation of cell death.…”

Section: Mitochondrial Fusion and Cell Deathmentioning

confidence: 99%

“…Interestingly, Drp1, Bax and Mfn2 have been shown to colocalize into discrete foci during apoptosis, suggesting that Mfn2 may be sequestered and inhibited during apoptosis [33]. Increased Mfn2 activity can inhibit Bax activation and cytochrome c release [69,79], whereas the lack of Mfn2 activity sensitize cells to apoptotic stimuli [69]. In neuronal system, Barsoum and colleagues demonstrated that overexpression of Mfn1 can protect against NO induced neuronal cell death.…”

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: Mitochondrial Fusion Proteinsmentioning

confidence: 95%

Section: Mitochondrial Fusion and Cell Deathmentioning

confidence: 99%

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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“…The notion that mitochondrial fission is a step towards death is reinforced by the ability of overexpressed pro-fusion Mfn1 and Mfn2 to block apoptosis induced by stimuli that recruit the mitochondrial pathway, perhaps by interfering with Bax activation. 56,57 An open question is why increased fission accelerates cell death. A unifying model proposed by Shore and co-workers 58 implies cristae remodelling downstream of Drp1 activation, which in turn depends on mitochondrial Ca 2 þ uptake induced by the BH3-only molecule BIK.…”

Section: Function Follows Form: Consequences Of Mitochondrial Shape Cmentioning

confidence: 99%

A cut short to death: Parl and Opa1 in the regulation of mitochondrial morphology and apoptosis

Scorrano

2007

Cell Death Differ

131

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Mitochondria are crucial amplifiers of death signals. They release cytochrome c and other pro-apoptotic factors required to fully activate effector caspases. This release is accompanied by fragmentation of the mitochondrial reticulum and by remodelling of the internal structure of the organelle. Here we review data supporting the existence of a regulatory network in the inner mitochondrial membrane that includes optic atrophy 1 (Opa1), a dynamin-related protein, and presenilin-associated rhomboidlike (Parl), a rhomboid protease. Opa1 regulates remodelling of the cristae independent of its effect on fusion. Cristae remodelling conversely requires Parl, which participates in the production of a soluble form of Opa1 retrieved together with the integral membrane one in oligomers that are disrupted early during apoptosis. Parl itself is regulated by proteolysis to generate a cleaved form, which in turn modulates the shape of the mitochondrial reticulum. Cleavage of Parl depends on its phosphorylation state around the cleavage site, implicating mitochondrial kinases and phosphatases in the regulation of mitochondrial shape.

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“…Continuous illumination of TMRM can trigger singlet oxygen ( 1 O 2 ) generation and thereby lead to photodynamic damage, opening of the mitochondrial permeability transition pore (PTP), and mitochondrial depolarization (11,(21)(22)(23)(24). Additionally, TMRM photobleaching during image acquisi- ORIGINAL ARTICLE tion might reduce the fluorescence signal in a Dw-independent manner.…”

Section: Relevance Of Tmrm-induced Photodamagementioning

confidence: 99%

Life cell quantification of mitochondrial membrane potential at the single organelle level

et al. 2007

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Mitochondrial membrane potential (Dw) is key to mitochondrial function and cellular survival. Here, we aimed to develop an automated protocol allowing sensitive quantification of Dw in living cells at the level of individual mitochondria. Human skin fibroblasts were stained with the fluorescent cation tetramethyl rhodamine methyl ester (TMRM), which is sequestered by mitochondria according to their Dw. Cells were visualized by videomicroscopy and the acquired images were processed to generate a mitochondria-specific mask. The latter was superimposed on the original image to allow quantification of TMRM fluorescence. Following validation, our approach revealed that mitochondria with different Dw coexisted within the same cell. Furthermore, our method allowed reproducible detection of small (\10%) reductions in TMRM intensity induced by the complex III inhibitor antimycin A. Mitochondrial uncoupling by p-trifluoromethoxy carbonyl cyanide phenyl hydrazone (FCCP) greatly reduced mitochondrial TMRM fluorescence. Under these conditions faithful mask calculation and TMRM intensity analysis were still possible using a mitochondria-targeted green fluorescence protein (mitoAcGFP1), expressed in the cells using baculoviral transfection. ' International Society for Analytical CytologyKey terms fibroblasts; TMRM; AcGFP1; image processing and analysis MITOCHONDRIA actively maintain a highly negative potential across their inner membrane (Dw), which is essential for mitochondrial function and cell viability. This potential is maintained by four protein complexes (CI-CIV) of the mitochondrial electron transport chain (ETC) that, together with the F 0 /F 1 -ATP-synthase (CV), constitute the oxidative phosphorylation (OXPHOS) system (1). Mitochondria are fuelled by pyruvate and fatty acids, which are used as carbon sources for the tricarboxylic acid cycle in the mitochondrial matrix. The products of this cycle, NADH and FADH 2 , subsequently feed electrons into the ETC at CI and CII, respectively. At three locations within the chain, CI, CIII, and CIV, the electron transport is used to expel protons from the matrix space to the intermembrane space. The H 1 ejection results in the establishment of an electrochemical H 1 gradient, which consists of a chemical (DpH) and electrical (Dw) component. At CV, protons are allowed to flow back into the mitochondrial matrix to drive the synthesis of ATP from ADP and inorganic phosphate (P i ). In intact respiring mitochondria, the ETC and ATP synthesis are efficiently coupled. Importantly, a large number of diseases have been linked to mitochondrial dysfunction, including age-related neurological diseases, cardiovascular disease, cancer and diabetes (reviewed in Refs. 2, 3).Since Dw is regarded as a key indicator of mitochondrial health and metabolic activity, the accurate determination of this parameter in intact cells is important to address many research questions. Most assays for monitoring Dw in living cells

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Activated Mitofusin 2 Signals Mitochondrial Fusion, Interferes with Bax Activation, and Reduces Susceptibility to Radical Induced Depolarization

Cited by 280 publications

References 55 publications

Mitochondrial dynamics in the regulation of neuronal cell death

Mitochondrial dynamics in the regulation of neuronal cell death

A cut short to death: Parl and Opa1 in the regulation of mitochondrial morphology and apoptosis

Life cell quantification of mitochondrial membrane potential at the single organelle level

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