The human dynamin‐related protein OPA1 is anchored to the mitochondrial inner membrane facing the inter‐membrane space

Olichon, Aurélien; Emorine, Laurent J.; Descoins, Eric; Pelloquin, Laetitia; Brichese, Laetitia; Gas, Nicole; Guillou, Emmanuelle; Delettre, Cécile; Valette, Annie; Hamel, Christian; Ducommun, Bernard; Lenaers, Guy; Bélenguer, Pascale

doi:10.1016/s0014-5793(02)02985-x

Cited by 371 publications

(301 citation statements)

References 31 publications

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“…Since whole embryo AIF knockouts are embryonic lethal, we generated conditional forebrain deficient AIF mice to study the role of AIF in neurons. We first observed that AIF −/− neurons exhibited fragmented mitochondria with dilated mitochondrial cristae and defective mitochondrial respiration, which is similar to Opa1 knockdown cells [132,145]. EM studies of neurons expressing the unreleasable form of AIF showed elongated mitochondria and tighter cristae tubules.…”

Section: Mitochondrial Cristae Structure and Cell Death: Demolition Fmentioning

confidence: 66%

“…The third GTPase required for mitochondrial fusion is localized to the intermembrane space and is called Opa1 [86][87][88][89]. Opa1 (Optical Atrophy 1) is imported into the mitochondrial inner membrane where it undergoes a regulated cleavage event to release a soluble shorter form of the protein into the intermembrane space.…”

Section: Mitochondrial Fusion Proteinsmentioning

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 Cristae Structure and Cell Death: Demolition Fmentioning

confidence: 66%

Section: Mitochondrial Fusion Proteinsmentioning

confidence: 99%

Mitochondrial dynamics in the regulation of neuronal cell death

2007

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“…OPA1 and its orthologues, encoded by a single nuclear gene, are the only proteins belonging to the dynamin family that are located inside mitochondria. 7,24,25 In yeast, Mgm1 appears in Western blots as doublet, the fast migrating form resulting from the cleavage by a mitochondrial rhomboid-like protease of the slow migrating form. 26,27 In human and mouse cell lines, previous works have reported the presence of 2-5 different electrophoretic forms of the OPA1 protein, 7,11,19 which also result from different proteolytic cleavages.…”

Section: Resultsmentioning

confidence: 99%

“…[1][2][3] The outer and inner mitochondrial membrane (OMM and IMM) dynamics crosstalk and involve large GTPases: respectively, the mitofusins Mfn1 and Mfn2 4,5 and the dynamin-related DRP1 6 on the OMM, and the dynaminrelated OPA1, localized in the inter membrane space (IMS). 7 Mitochondrial fission is tightly associated to the apoptotic process, and physical and functional interactions between apoptotic proteins including Bcl2-homologue domains and DRP1 and mitofusins have been identified. 8 In addition, BH3-only proapoptotic proteins, exemplified by tBid and Bik, might act directly on the IMM structure, although their intramitochondrial target remains unknown.…”

mentioning

confidence: 99%

OPA1 alternate splicing uncouples an evolutionary conserved function in mitochondrial fusion from a vertebrate restricted function in apoptosis

et al. 2006

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In most eucaryote cells, release of apoptotic proteins from mitochondria involves fission of the mitochondrial network and drastic remodelling of the cristae structures. The intramitochondrial dynamin OPA1, as a potential central actor of these processes, exists as eight isoforms resulting from the alternate splicing combinations of exons (Ex) 4, 4b and 5b, which functions remain undetermined. Here, we show that Ex4 that is conserved throughout evolution confers functions to OPA1 involved in the maintenance of the DW m and in the fusion of the mitochondrial network. Conversely, Ex4b and Ex5b, which are vertebrate specific, define a function involved in cytochrome c release, an apoptotic process also restricted to vertebrates. The drastic changes of OPA1 variant abundance in different organs suggest that nuclear splicing can control mitochondrial dynamic fate and susceptibility to apoptosis and pathologies. Mitochondrial membrane dynamics, involving both the fusionfission of the mitochondrial network and remodelling of cristae structures, are essential processes in cellular adaptation to changes of growth condition and programmed cell death. [1][2][3] The outer and inner mitochondrial membrane (OMM and IMM) dynamics crosstalk and involve large GTPases: respectively, the mitofusins Mfn1 and Mfn2 4,5 and the dynamin-related DRP1 6 on the OMM, and the dynaminrelated OPA1, localized in the inter membrane space (IMS). 7 Mitochondrial fission is tightly associated to the apoptotic process, and physical and functional interactions between apoptotic proteins including Bcl2-homologue domains and DRP1 and mitofusins have been identified. 8 In addition, BH3-only proapoptotic proteins, exemplified by tBid and Bik, might act directly on the IMM structure, although their intramitochondrial target remains unknown. 3,9 Further crosstalk between the OMM and the IMM is exemplified by the OMM fission and fusion regulation by the mitochondrial membrane potential (DC m ) 10 and structural integrity 11 and by interaction between OPA1 and Mfn1. 12 The IMM forms, an architecturally complex structure, that has been reconsidered recently in the light of tomography analysis associated to transmission electron microscopy (TEM). Indeed, tubular inner membrane junctions, called cristae junctions, have been evidenced between the IMM facing the OMM and the vesicular-shaped cristae. 13 In vertebrate cells, during the apoptotic process, the cristae junction topology is drastically modified to mobilize cytochrome c (cyt c) from the intracristae compartment to the IMS, before its extensive release in the cytoplasm. 3,9 How this process is physically controlled and related to the OMM dynamic remains unknown. We and others have shown that OPA1 is a good candidate for the regulation of the cristae structure in the mitochondria. 11,14 Indeed, downregulation of OPA1 affect the IMM structure and integrity, leading to respiration defects and DC m loss, fission of the mitochondrial network, impairment of growth and apoptosis 11,14-18 and OPA1 overexpressio...

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“…79,80 It should be noted that Paraplegin faces the matrix and that the mitochondrial processing peptidase already trims most of the matrix residues of Opa1. 81 At this stage a plausible scenario deserving further investigation is that Paraplegin and Parl somehow cooperate in the cleavage of Opa1. For example, Paraplegin (or one of the other mAAA proteases that form the mAAA complex with paraplegin 82 ) could participate in the activation of Parl at the level of its N-terminal Pb domain.…”

Section: Parl: a Shortcut To Regulate Apoptosismentioning

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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The human dynamin‐related protein OPA1 is anchored to the mitochondrial inner membrane facing the inter‐membrane space

Cited by 371 publications

References 31 publications

Mitochondrial dynamics in the regulation of neuronal cell death

Mitochondrial dynamics in the regulation of neuronal cell death

OPA1 alternate splicing uncouples an evolutionary conserved function in mitochondrial fusion from a vertebrate restricted function in apoptosis

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

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