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1. Mutant huntingtin impairs neurodevelopment in human brain organoids through CHCHD2-mediated neurometabolic failure

Author

Lisowski, Pawel, Lickfett, Selene, Rybak-Wolf, Agnieszka, Menacho, Carmen, Le, Stephanie, Pentimalli, Tancredi Massimo, Notopoulou, Sofia, Dykstra, Werner, Oehler, Daniel, López-Calcerrada, Sandra, Mlody, Barbara, Otto, Maximilian, Wu, Haijia, Richter, Yasmin, Roth, Philipp, Anand, Ruchika, Kulka, Linda A. M., Meierhofer, David, Glazar, Petar, Legnini, Ivano, Telugu, Narasimha Swamy, Hahn, Tobias, Neuendorf, Nancy, Miller, Duncan C., Böddrich, Annett, Polzin, Amin, Mayatepek, Ertan, Diecke, Sebastian, Olzscha, Heidi, Kirstein, Janine, Ugalde, Cristina, Petrakis, Spyros, Cambridge, Sidney, Rajewsky, Nikolaus, Kühn, Ralf, Wanker, Erich E., Priller, Josef, Metzger, Jakob J., and Prigione, Alessandro

Published
2024
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4. Molecular and cellular evidence for the impact of a hypertrophic cardiomyopathy-associated RAF1 variant on the structure and function of contractile machinery in bioartificial cardiac tissues

Author

Nakhaei-Rad, Saeideh, Haghighi, Fereshteh, Bazgir, Farhad, Dahlmann, Julia, Busley, Alexandra Viktoria, Buchholzer, Marcel, Kleemann, Karolin, Schänzer, Anne, Borchardt, Andrea, Hahn, Andreas, Kötter, Sebastian, Schanze, Denny, Anand, Ruchika, Funk, Florian, Kronenbitter, Annette Vera, Scheller, Jürgen, Piekorz, Roland P., Reichert, Andreas S., Volleth, Marianne, Wolf, Matthew J., Cirstea, Ion Cristian, Gelb, Bruce D., Tartaglia, Marco, Schmitt, Joachim P., Krüger, Martina, Kutschka, Ingo, Cyganek, Lukas, Zenker, Martin, Kensah, George, and Ahmadian, Mohammad R.

Published
2023
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5. NECAB2 is an endosomal protein important for striatal function

Author

Bueno, Diones, Narayan Dey, Partha, Schacht, Teresa, Wolf, Christina, Wüllner, Verena, Morpurgo, Elena, Rojas-Charry, Liliana, Sessinghaus, Lena, Leukel, Petra, Sommer, Clemens, Radyushkin, Konstantin, Florin, Luise, Baumgart, Jan, Stamm, Paul, Daiber, Andreas, Horta, Guilherme, Nardi, Leonardo, Vasic, Verica, Schmeisser, Michael J., Hellwig, Andrea, Oskamp, Angela, Bauer, Andreas, Anand, Ruchika, Reichert, Andreas S., Ritz, Sandra, Nocera, Gianluigi, Jacob, Claire, Peper, Jonas, Silies, Marion, Frauenknecht, Katrin B.M., Schäfer, Michael K.E., and Methner, Axel

Published
2023
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7. The mycotoxin phomoxanthone A disturbs the form and function of the inner mitochondrial membrane.

Author

Böhler, Philip, Stuhldreier, Fabian, Anand, Ruchika, Kondadi, Arun Kumar, Schlütermann, David, Berleth, Niklas, Deitersen, Jana, Wallot-Hieke, Nora, Wu, Wenxian, Frank, Marian, Niemann, Hendrik, Wesbuer, Elisabeth, Barbian, Andreas, Luyten, Tomas, Parys, Jan B, Weidtkamp-Peters, Stefanie, Borchardt, Andrea, Reichert, Andreas S, Peña-Blanco, Aida, García-Sáez, Ana J, Itskanov, Samuel, van der Bliek, Alexander M, Proksch, Peter, Wesselborg, Sebastian, and Stork, Björn

Subjects
Cell Line, Mitochondria, Animals, Humans, Mice, Ascomycota, Calcium, Xanthones, Electron Transport Chain Complex Proteins, Mycotoxins, Electron Transport, Mitochondrial Membranes, Biochemistry and Cell Biology, Oncology and Carcinogenesis
Abstract

Mitochondria are cellular organelles with crucial functions in the generation and distribution of ATP, the buffering of cytosolic Ca2+ and the initiation of apoptosis. Compounds that interfere with these functions are termed mitochondrial toxins, many of which are derived from microbes, such as antimycin A, oligomycin A, and ionomycin. Here, we identify the mycotoxin phomoxanthone A (PXA), derived from the endophytic fungus Phomopsis longicolla, as a mitochondrial toxin. We show that PXA elicits a strong release of Ca2+ from the mitochondria but not from the ER. In addition, PXA depolarises the mitochondria similarly to protonophoric uncouplers such as CCCP, yet unlike these, it does not increase but rather inhibits cellular respiration and electron transport chain activity. The respiration-dependent mitochondrial network structure rapidly collapses into fragments upon PXA treatment. Surprisingly, this fragmentation is independent from the canonical mitochondrial fission and fusion mediators DRP1 and OPA1, and exclusively affects the inner mitochondrial membrane, leading to cristae disruption, release of pro-apoptotic proteins, and apoptosis. Taken together, our results suggest that PXA is a mitochondrial toxin with a novel mode of action that might prove a useful tool for the study of mitochondrial ion homoeostasis and membrane dynamics.

Published
2018

12. Mutant huntingtin impairs neurodevelopment in human brain organoids through CHCHD2-mediated neurometabolic failure

Author

TN groep Hol, Brain, Lisowski, Pawel, Lickfett, Selene, Rybak-Wolf, Agnieszka, Menacho, Carmen, Le, Stephanie, Pentimalli, Tancredi Massimo, Notopoulou, Sofia, Dykstra, Werner, Oehler, Daniel, López-Calcerrada, Sandra, Mlody, Barbara, Otto, Maximilian, Wu, Haijia, Richter, Yasmin, Roth, Philipp, Anand, Ruchika, Kulka, Linda A.M., Meierhofer, David, Glazar, Petar, Legnini, Ivano, Telugu, Narasimha Swamy, Hahn, Tobias, Neuendorf, Nancy, Miller, Duncan C., Böddrich, Annett, Polzin, Amin, Mayatepek, Ertan, Diecke, Sebastian, Olzscha, Heidi, Kirstein, Janine, Ugalde, Cristina, Petrakis, Spyros, Cambridge, Sidney, Rajewsky, Nikolaus, Kühn, Ralf, Wanker, Erich E., Priller, Josef, Metzger, Jakob J., Prigione, Alessandro, TN groep Hol, Brain, Lisowski, Pawel, Lickfett, Selene, Rybak-Wolf, Agnieszka, Menacho, Carmen, Le, Stephanie, Pentimalli, Tancredi Massimo, Notopoulou, Sofia, Dykstra, Werner, Oehler, Daniel, López-Calcerrada, Sandra, Mlody, Barbara, Otto, Maximilian, Wu, Haijia, Richter, Yasmin, Roth, Philipp, Anand, Ruchika, Kulka, Linda A.M., Meierhofer, David, Glazar, Petar, Legnini, Ivano, Telugu, Narasimha Swamy, Hahn, Tobias, Neuendorf, Nancy, Miller, Duncan C., Böddrich, Annett, Polzin, Amin, Mayatepek, Ertan, Diecke, Sebastian, Olzscha, Heidi, Kirstein, Janine, Ugalde, Cristina, Petrakis, Spyros, Cambridge, Sidney, Rajewsky, Nikolaus, Kühn, Ralf, Wanker, Erich E., Priller, Josef, Metzger, Jakob J., and Prigione, Alessandro

Published
2024

14. Mitochondrial Apolipoprotein MIC26 is a metabolic rheostat regulating central cellular fuel pathways

Author

Lubeck, Melissa, primary, Naha, Ritam, additional, Schaumkessel, Yulia, additional, Westhoff, Philipp, additional, Stefanski, Anja, additional, Petzsch, Patrick, additional, Stühler, Kai, additional, Köhrer, Karl, additional, Weber, Andreas P. M., additional, Anand, Ruchika, additional, Reichert, Andreas S., additional, and Kondadi, Arun Kumar, additional

Published
2023
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23. SLP2 coordinates MICOS assembly and cristae morphogenesis via MIC13 and YME1L

Author

Naha, Ritam, Strohm, Rebecca, Urbach, Jennifer, Wittig, Ilka, Reichert, Andreas, Kondadi, Arun Kumar, Anand, Ruchika, Naha, Ritam, Strohm, Rebecca, Urbach, Jennifer, Wittig, Ilka, Reichert, Andreas, Kondadi, Arun Kumar, and Anand, Ruchika

Abstract

The MICOS complex subunit MIC13 is essential for mitochondrial cristae organization. Mutations in MIC13 cause severe mitochondrial hepato-encephalopathy displaying defective cristae morphology and loss of the MIC10-subcomplex. Here we identified SLP2 as a novel interacting partner of MIC13 and decipher a critical role of SLP2 for MICOS assembly at distinct steps. SLP2 provides a large interaction hub for MICOS subunits and loss of SLP2 imparted YME1L-mediated proteolysis of MIC26 and drastic alterations in cristae morphology. We further identified a MIC13-specific role in stabilizing the MIC10-subcomplex via a MIC13-YME1L axis. SLP2 together with the stabilized MIC10-subcomplex promotes efficient assembly of the MIC60-subcomplex forming the MICOS-MIB complex. Consistently, super-resolution nanoscopy showed a dispersed distribution of the MIC60 in cells lacking SLP2 and MIC13. Our study reveals converging and interdependent assembly pathways for the MIC10- and MIC60-subcomplexes which are controlled in two ways, the MIC13-YME1L and the SLP2-YME1L axes, revealing mechanistic insights of these factors in cristae morphogenesis. These results will be helpful in understanding the human pathophysiology linked to mutations in MIC13 or its interaction partners.

Published
2023

24. MIC13 and SLP2 seed the assembly of MIC60-subcomplex to facilitate crista junction formation

Author

Naha, Ritam, Strohm, Rebecca, Urbach, Jennifer, Wittig, Ilka, Reichert, Andreas, Kondadi, Arun Kumar, Anand, Ruchika, Naha, Ritam, Strohm, Rebecca, Urbach, Jennifer, Wittig, Ilka, Reichert, Andreas, Kondadi, Arun Kumar, and Anand, Ruchika

Abstract

The MICOS complex subunit MIC13 is essential for mitochondrial cristae organization. Mutations in MIC13 cause severe mitochondrial hepato-encephalopathy displaying defective cristae morphology and loss of the MIC10-subcomplex. Here we identified stomatin-like protein 2 (SLP2) as an interacting partner of MIC13 and decipher a critical role of SLP2 as an auxiliary MICOS subunit, modulating cristae morphology. SLP2 provides a large interaction hub for MICOS subunits and loss of SLP2 leads to drastic alterations in cristae morphology. Double deletion of SLP2 and MIC13 showed reduced assembly of core MICOS subunit, MIC60 into MICOS and dispersion of MIC60-specific puncta, demonstrating a critical role of SLP2-MIC13 in MICOS assembly and crista junction (CJ) formation. We further identified that the mitochondrial i-AAA protease YME1L in coordination either with MIC13 or SLP2 differentially regulates MICOS assembly pathways thereby interlinking MIC13-specific or scaffolding-specific role of SLP2 with quality control and assembly of the MICOS complex. YME1L- depletion in MIC13 KO could restore MIC10-subcomplex and reform the nascent CJ. Taken together, we propose ‘seeder’ model for MICOS assembly and CJ formation, where SLP2- MIC13 seed the assembly of MIC60 into MICOS complex and promote the formation of CJ by regulating the quality and stability of MIC10-subcomplex.

Published
2023

28. MIC26 and MIC27 are bona fide subunits of the MICOS complex in mitochondria and do not exist as glycosylated apolipoproteins.

Author

Lubeck, Melissa, Derkum, Nick H., Naha, Ritam, Strohm, Rebecca, Driessen, Marc D., Belgardt, Bengt-Frederik, Roden, Michael, Stühler, Kai, Anand, Ruchika, Reichert, Andreas S., and Kondadi, Arun Kumar

Subjects
APOLIPOPROTEINS, MEMBRANE proteins, MITOCHONDRIA, MITOCHONDRIAL membranes, MASS spectrometry
Abstract

Impairments of mitochondrial functions are linked to human ageing and pathologies such as cancer, cardiomyopathy, neurodegeneration and diabetes. Specifically, aberrations in ultrastructure of mitochondrial inner membrane (IM) and factors regulating them are linked to diabetes. The development of diabetes is connected to the 'Mitochondrial Contact Site and Cristae Organising System' (MICOS) complex which is a large membrane protein complex defining the IM architecture. MIC26 and MIC27 are homologous apolipoproteins of the MICOS complex. MIC26 has been reported as a 22 kDa mitochondrial and a 55 kDa glycosylated and secreted protein. The molecular and functional relationship between these MIC26 isoforms has not been investigated. In order to understand their molecular roles, we depleted MIC26 using siRNA and further generated MIC26 and MIC27 knockouts (KOs) in four different human cell lines. In these KOs, we used four anti-MIC26 antibodies and consistently detected the loss of mitochondrial MIC26 (22 kDa) and MIC27 (30 kDa) but not the loss of intracellular or secreted 55 kDa protein. Thus, the protein assigned earlier as 55 kDa MIC26 is nonspecific. We further excluded the presence of a glycosylated, high-molecular weight MIC27 protein. Next, we probed GFP- and myc-tagged variants of MIC26 with antibodies against GFP and myc respectively. Again, only the mitochondrial versions of these tagged proteins were detected but not the corresponding high-molecular weight MIC26, suggesting that MIC26 is indeed not post-translationally modified. Mutagenesis of predicted glycosylation sites in MIC26 also did not affect the detection of the 55 kDa protein band. Mass spectrometry of a band excised from an SDS gel around 55 kDa could not confirm the presence of any peptides derived from MIC26. Taken together, we conclude that both MIC26 and MIC27 are exclusively localized in mitochondria and that the observed phenotypes reported previously are exclusively due to their mitochondrial function. [ABSTRACT FROM AUTHOR]

Published
2023
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29. Alteration of myocardial structure and function in RAF1-associated Noonan syndrome: Insights from cardiac disease modeling based on patient-derived iPSCs

Author

Nakhaei-Rad, Saeideh, primary, Bazgir, Farhad, additional, Dahlmann, Julia, additional, Busley, Alexandra Viktoria, additional, Buchholzer, Marcel, additional, Haghighi, Fereshteh, additional, Schänzer, Anne, additional, Hahn, Andreas, additional, Kötter, Sebastian, additional, Schanze, Denny, additional, Anand, Ruchika, additional, Funk, Florian, additional, Borchardt, Andrea, additional, Kronenbitter, Annette Vera, additional, Scheller, Jürgen, additional, Piekorz, Roland P., additional, Reichert, Andreas S., additional, Volleth, Marianne, additional, Wolf, Matthew J., additional, Cirstea, Ion Cristian, additional, Gelb, Bruce D., additional, Tartaglia, Marco, additional, Schmitt, Joachim, additional, Krüger, Martina, additional, Kutschka, Ingo, additional, Cyganek, Lukas, additional, Zenker, Martin, additional, Kensah, George, additional, and Ahmadian, Mohammad R., additional

Published
2022
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31. Emerging Roles of the MICOS Complex in Cristae Dynamics and Biogenesis

Author

Anand, Ruchika, Reichert, Andreas S., and Kondadi, Arun Kumar

Subjects
mitochondria, cristae biogenesis, cristae dynamics, QH301-705.5, cristae, Review, Biology (General), MICOS
Abstract

Simple Summary Mitochondria possess an outer and inner membrane. The part of the inner membrane parallel to the outer membrane is termed the inner boundary membrane, while the cristae membrane folds towards the mitochondrial matrix and houses the respiratory chain complexes. Crista junctions are located at the interface of the inner boundary membrane and the cristae membrane and contain the important ‘mitochondrial contact site and cristae organizing system’ complex. Despite the growing evidence that the mitochondrial inner membrane could remodel, cristae membranes were largely considered static for nearly seventy years, as the observations were mostly based on electron microscopy and tomography. Recently, using fluorescence super-resolution techniques, several studies showed that cristae membranes undergo dynamic remodeling in living cells, and probably even fission and fusion of the inner membrane. In this review, we discuss the important recent literature conveying the emerging role of the MICOS complex in cristae dynamics and its relation to cristae biogenesis. As the aberrant inner membrane architecture is connected to various pathologies such as cardiomyopathies, neurodegeneration and diabetes, understanding the roles of various molecules connected with cristae biogenesis and dynamics would shed light on the pathophysiology, probably leading to therapeutics in the near future. Abstract Mitochondria are double membrane-enclosed organelles performing important cellular and metabolic functions such as ATP generation, heme biogenesis, apoptosis, ROS production and calcium buffering. The mitochondrial inner membrane (IM) is folded into cristae membranes (CMs) of variable shapes using molecular players including the ‘mitochondrial contact site and cristae organizing system’ (MICOS) complex, the dynamin-like GTPase OPA1, the F1FO ATP synthase and cardiolipin. Aberrant cristae structures are associated with different disorders such as diabetes, neurodegeneration, cancer and hepato-encephalopathy. In this review, we provide an updated view on cristae biogenesis by focusing on novel roles of the MICOS complex in cristae dynamics and shaping of cristae. For over seven decades, cristae were considered as static structures. It was recently shown that cristae constantly undergo rapid dynamic remodeling events. Several studies have re-oriented our perception on the dynamic internal ambience of mitochondrial compartments. In addition, we discuss the recent literature which sheds light on the still poorly understood aspect of cristae biogenesis, focusing on the role of MICOS and its subunits. Overall, we provide an integrated and updated view on the relation between the biogenesis of cristae and the novel aspect of cristae dynamics.

Published
2021

32. NECAB2 participates in an endosomal pathway of mitochondrial stress response at striatal synapses

Author

Bueno, Diones, primary, Narayan Dey, Partha, additional, Schacht, Teresa, additional, Wolf, Christina, additional, Wüllner, Verena, additional, Morpurgo, Elena, additional, Rojas-Charry, Liliana, additional, Sessinghaus, Lena, additional, Leukel, Petra, additional, Sommer, Clemens, additional, Radyushkin, Konstantin, additional, Schaefer, Michael, additional, Florin, Luise, additional, Baumgart, Jan, additional, Stamm, Paul, additional, Daiber, Andreas, additional, Horta, Guilherme, additional, Nardi, Leonardo, additional, Vasic, Verica, additional, Schmeisser, Michael J., additional, Hellwig, Andrea, additional, Oskamp, Angela, additional, Bauer, Andreas, additional, Anand, Ruchika, additional, Reichert, Andreas S., additional, Ritz, Sandra, additional, Nocera, Gianluigi, additional, Jacob, Claire, additional, Peper, Jonas, additional, Silies, Marion, additional, Frauenknecht, Katrin B. M., additional, and Methner, Axel, additional

Published
2021
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34. MIC26 and MIC27 cooperate to regulate cardiolipin levels and the landscape of OXPHOS complexes

Author

Anand, Ruchika, primary, Kondadi, Arun Kumar, additional, Meisterknecht, Jana, additional, Golombek, Mathias, additional, Nortmann, Oliver, additional, Riedel, Julia, additional, Peifer-Weiß, Leon, additional, Brocke-Ahmadinejad, Nahal, additional, Schlütermann, David, additional, Stork, Björn, additional, Eichmann, Thomas O, additional, Wittig, Ilka, additional, and Reichert, Andreas S, additional

Published
2020
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37. Correction: SIRT4 interacts with OPA1 and regulates mitochondrial quality control and mitophagy

Author

Lang, Alexander, primary, Anand, Ruchika, additional, Altinoluk-Hambüchen, Simone, additional, Ezzahoini, Hakima, additional, Stefanski, Anja, additional, Iram, Afshin, additional, Bergmann, Laura, additional, Urbach, Jennifer, additional, Böhler, Philip, additional, Hänsel, Jan, additional, Franke, Manuel, additional, Stühler, Kai, additional, Krutmann, Jean, additional, Scheller, Jürgen, additional, Stork, Björn, additional, Reichert, Andreas S., additional, and Piekorz, Roland P., additional

Published
2018
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39. SIRT4 interacts with OPA1 and regulates mitochondrial quality control and mitophagy

Author

Lang, Alexander, primary, Anand, Ruchika, additional, Altinoluk-Hambüchen, Simone, additional, Ezzahoini, Hakima, additional, Stefanski, Anja, additional, Iram, Afshin, additional, Bergmann, Laura, additional, Urbach, Jennifer, additional, Böhler, Philip, additional, Hänsel, Jan, additional, Franke, Manuel, additional, Stühler, Kai, additional, Krutmann, Jean, additional, Scheller, Jürgen, additional, Stork, Björn, additional, Reichert, Andreas S., additional, and Piekorz, Roland P., additional

Published
2017
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40. Mic13 is essential for formation of crista junctions in mammalian cells

Author

Anand, Ruchika, Strecker, Valentina, Urbach, Jennifer, Wittig, Ilka, Reichert, Andreas, Anand, Ruchika, Strecker, Valentina, Urbach, Jennifer, Wittig, Ilka, and Reichert, Andreas

Abstract

Mitochondrial cristae are connected to the inner boundary membrane via crista junctions which are implicated in the regulation of oxidative phosphorylation, apoptosis, and import of lipids and proteins. The MICOS complex determines formation of crista junctions. We performed complexome profiling and identified Mic13, also termed Qil1, as a subunit of the MICOS complex. We show that MIC13 is an inner membrane protein physically interacting with MIC60, a central subunit of the MICOS complex. Using the CRISPR/Cas method we generated the first cell line deleted for MIC13. These knockout cells show a complete loss of crista junctions demonstrating that MIC13 is strictly required for the formation of crista junctions. MIC13 is required for the assembly of MIC10, MIC26, and MIC27 into the MICOS complex. However, it is not needed for the formation of the MIC60/MIC19/MIC25 subcomplex suggesting that the latter is not sufficient for crista junction formation. MIC13 is also dispensable for assembly of respiratory chain complexes and for maintaining mitochondrial network morphology. Still, lack of MIC13 resulted in a moderate reduction of mitochondrial respiration. In summary, we show that MIC13 has a fundamental role in crista junction formation and that assembly of respiratory chain supercomplexes is independent of mitochondrial cristae shape.

Published
2016

42. The i-AAA protease YME1L and OMA1 cleave OPA1 to balance mitochondrial fusion and fission

Author

Anand, Ruchika, Wai, Timothy, Baker, Michael J., Kladt, Nikolay, Schauss, Astrid C., Rugarli, Elena, Langer, Thomas, Anand, Ruchika, Wai, Timothy, Baker, Michael J., Kladt, Nikolay, Schauss, Astrid C., Rugarli, Elena, and Langer, Thomas

Abstract

Mitochondrial fusion and structure depend on the dynamin-like GTPase OPA1, whose activity is regulated by proteolytic processing. Constitutive OPA1 cleavage by YME1L and OMA1 at two distinct sites leads to the accumulation of both long and short forms of OPA1 and maintains mitochondrial fusion. Stress-induced OPA1 processing by OMA1 converts OPA1 completely into short isoforms, inhibits fusion, and triggers mitochondrial fragmentation. Here, we have analyzed the function of different OPA1 forms in cells lacking YME1L, OMA1, or both. Unexpectedly, deletion of Oma1 restored mitochondrial tubulation, cristae morphogenesis, and apoptotic resistance in cells lacking YME1L. Long OPA1 forms were sufficient to mediate mitochondrial fusion in these cells. Expression of short OPA1 forms promoted mitochondrial fragmentation, which indicates that they are associated with fission. Consistently, GTPase-inactive, short OPA1 forms partially colocalize with ER-mitochondria contact sites and the mitochondrial fission machinery. Thus, OPA1 processing is dispensable for fusion but coordinates the dynamic behavior of mitochondria and is crucial for mitochondrial integrity and quality control.

Published
2014

43. Stress-induced OMA1 activation and autocatalytic turnover regulate OPA1-dependent mitochondrial dynamics

Author

Baker, Michael J., Lampe, Philipp A., Stojanovski, Diana, Korwitz, Anne, Anand, Ruchika, Tatsuta, Takashi, Langer, Thomas, Baker, Michael J., Lampe, Philipp A., Stojanovski, Diana, Korwitz, Anne, Anand, Ruchika, Tatsuta, Takashi, and Langer, Thomas

Abstract

The dynamic network of mitochondria fragments under stress allowing the segregation of damaged mitochondria and, in case of persistent damage, their selective removal by mitophagy. Mitochondrial fragmentation upon depolarisation of mitochondria is brought about by the degradation of central components of the mitochondrial fusion machinery. The OMA1 peptidase mediates the degradation of long isoforms of the dynamin-like GTPase OPA1 in the inner membrane. Here, we demonstrate that OMA1-mediated degradation of OPA1 is a general cellular stress response. OMA1 is constitutively active but displays strongly enhanced activity in response to various stress insults. We identify an amino terminal stress-sensor domain of OMA1, which is only present in homologues of higher eukaryotes and which modulates OMA1 proteolysis and activation. OMA1 activation is associated with its autocatalyic degradation, which initiates from both termini of OMA1 and results in complete OMA1 turnover. Autocatalytic proteolysis of OMA1 ensures the reversibility of the response and allows OPA1-mediated mitochondrial fusion to resume upon alleviation of stress. This differentiated stress response maintains the functional integrity of mitochondria and contributes to cell survival.

Published
2014

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