Literature DB >> 15878839

Discrimination between two steps in the mitochondrial permeability transition process.

Fernanda Ricchelli1, Giulio Jori, Silvano Gobbo, Peter Nikolov, Valeria Petronilli.   

Abstract

It is well known that a lag phase generally elapses between the addition of inducers of the mitochondrial permeability transition and the opening of the pore. To advance our present understanding as regards the significance of this phenomenon, we used experimental approaches which are sensitive to different aspects of the permeability transition process. The pore conformation was sensed by the fluorescence anisotropy changes of hematoporphyrin-labelled mitochondria. Membrane permeabilization was ascertained by following the matrix swelling consequent to external solute equilibration. We show that the anisotropy changes of mitochondria-bound hematoporphyrin precede both membrane depolarization (proton permeation) and matrix swelling (solute permeation), thus sensing a step of the permeability transition process that involves the pore in its closed state. We suggest that the opening of the pore is preceded by a structural remodelling of mitochondrial domains containing hematoporphyrin-near, pore-regulating histidines. Such a perturbation is strongly inhibited at acidic matrix pH and completely blocked by cyclosporin A. In sucrose-based media the opening of the pore can be strongly delayed, as compared to salt-based media, a fact which probably reflects perturbation of mitochondrial membranes by sugar. We conclude that the mitochondrial permeability transition could be described as an at least two-step process which is mainly regulated by conformational changes of the pore components.

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Year:  2005        PMID: 15878839     DOI: 10.1016/j.biocel.2005.04.001

Source DB:  PubMed          Journal:  Int J Biochem Cell Biol        ISSN: 1357-2725            Impact factor:   5.085


  11 in total

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5.  Toxicity of Pb2+ on rat liver mitochondria induced by oxidative stress and mitochondrial permeability transition.

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7.  Surface functional groups affect CdTe QDs behavior at mitochondrial level.

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8.  Spectroscopic, Polarographic, and Microcalorimetric Studies on Mitochondrial Dysfunction Induced by Ethanol.

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9.  Mitochondrial dysfunction induced by honokiol.

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10.  Mitochondrial morphology and function impaired by dimethyl sulfoxide and dimethyl Formamide.

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