Mitochondrial distribution and morphology depend on MDM33, a Saccharomyces cerevisiae gene encoding a novel protein of the mitochondrial inner membrane. Cells lacking Mdm33 contain ring-shaped, mostly interconnected mitochondria, which are able to form large hollow spheres. On the ultrastructural level, these aberrant organelles display extremely elongated stretches of outer and inner membranes enclosing a very narrow matrix space. Dilated parts of Δmdm33 mitochondria contain well-developed cristae. Overexpression of Mdm33 leads to growth arrest, aggregation of mitochondria, and generation of aberrant inner membrane structures, including septa, inner membrane fragments, and loss of inner membrane cristae. The MDM33 gene is required for the formation of net-like mitochondria in mutants lacking components of the outer membrane fission machinery, and mitochondrial fusion is required for the formation of extended ring-like mitochondria in cells lacking the MDM33 gene. The Mdm33 protein assembles into an oligomeric complex in the inner membrane where it performs homotypic protein–protein interactions. Our results indicate that Mdm33 plays a distinct role in the mitochondrial inner membrane to control mitochondrial morphology. We propose that Mdm33 is involved in fission of the mitochondrial inner membrane.
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17 February 2003
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February 18 2003
The inner membrane protein Mdm33 controls mitochondrial morphology in yeast
Marlies Messerschmitt,
Marlies Messerschmitt
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
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Stefan Jakobs,
Stefan Jakobs
2High Resolution Optical Microscopy Group, Max-Planck-Institut für Biophysikalische Chemie, D-37077 Göttingen, Germany
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Frank Vogel,
Frank Vogel
3Electron Microscopy Group, Max-Delbrück-Centrum für Molekulare Medizin, D-13092 Berlin, Germany
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Stefan Fritz,
Stefan Fritz
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
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Kai Stefan Dimmer,
Kai Stefan Dimmer
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
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Walter Neupert,
Walter Neupert
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
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Benedikt Westermann
Benedikt Westermann
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
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Marlies Messerschmitt
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
Stefan Jakobs
2High Resolution Optical Microscopy Group, Max-Planck-Institut für Biophysikalische Chemie, D-37077 Göttingen, Germany
Frank Vogel
3Electron Microscopy Group, Max-Delbrück-Centrum für Molekulare Medizin, D-13092 Berlin, Germany
Stefan Fritz
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
Kai Stefan Dimmer
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
Walter Neupert
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
Benedikt Westermann
1Institut für Physiologische Chemie, Universität München, D-81377 München, Germany
Address correspondence to Benedikt Westermann, Institut für Physiologische Chemie, Universität München, Butenandtstr. 5, D-81377 München, Germany. Tel.: 49-89-2180-77122. Fax: 49-89-2180-77093. E-mail: [email protected]
The online version of this article includes supplemental material.
*
Abbreviations used in this paper: cRFP, cytosolic red fluorescent protein; mtDNA, mitochondrial DNA; mtGFP, mitochondrial matrix–targeted GFP.
Received:
November 25 2002
Revision Received:
January 07 2003
Accepted:
January 07 2003
Online ISSN: 1540-8140
Print ISSN: 0021-9525
The Rockefeller University Press
2003
J Cell Biol (2003) 160 (4): 553–564.
Article history
Received:
November 25 2002
Revision Received:
January 07 2003
Accepted:
January 07 2003
Citation
Marlies Messerschmitt, Stefan Jakobs, Frank Vogel, Stefan Fritz, Kai Stefan Dimmer, Walter Neupert, Benedikt Westermann; The inner membrane protein Mdm33 controls mitochondrial morphology in yeast . J Cell Biol 17 February 2003; 160 (4): 553–564. doi: https://doi.org/10.1083/jcb.200211113
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