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Literature DB >> 11080247

Mitochondrial intermembrane junctional complexes and their role in cell death.

Abstract

A mitochondrial complex comprising the voltage-dependent anion channel (outer membrane), the adenine nucleotide translocase (inner membrane) and cyclophilin-D (matrix) assembles at contact sites between the inner and outer membranes. Under pathological conditions associated with ischaemia and reperfusion the junctional complex 'deforms' into the permeability transition (PT) pore, which can open transiently, allowing free permeation of low Mr solutes across the inner membrane. This may be a critical step in the pathogenesis of lethal cell injury in ischaemia and reperfusion. Moreover, it is argued, the degree of pore opening may be an important determinant of the relative extent of apoptosis and necrosis under these conditions. In addition, mitochondria are the major sites of action of Bax and other apoptotic regulatory proteins of the Bcl-2 family. These proteins control a mitochondrial amplificatory loop in the apoptotic signalling pathway in which cytochrome c and other apoptogenic proteins of the mitochondrial intermembrane space are released into the cytosol. There are indications that the junctional complex, or components of it, may also mediate the action of Bax, but in a way that does not involve PT pore formation.

Entities: Disease Gene

Mesh：

Substances：
Proteins

Year: 2000 PMID： 11080247 PMCID： PMC2270179 DOI： 10.1111/j.1469-7793.2000.00011.x

Source DB: PubMed Journal: J Physiol ISSN： 0022-3751 Impact factor: 5.182

87 in total

1. A heart mitochondrial Ca2(+)-dependent pore of possible relevance to re-perfusion-induced injury. Evidence that ADP facilitates pore interconversion between the closed and open states.

Authors: M Crompton; A Costi
Journal: Biochem J Date: 1990-02-15 Impact factor: 3.857

2. Evidence for the presence of a reversible Ca2+-dependent pore activated by oxidative stress in heart mitochondria.

Authors: M Crompton; A Costi; L Hayat
Journal: Biochem J Date: 1987-08-01 Impact factor: 3.857

3. Role of phosphocreatine in energy transport in skeletal muscle of bullfrog studied by 31P-NMR.

Authors: K Yoshizaki; H Watari; G K Radda
Journal: Biochim Biophys Acta Date: 1990-02-19

4. Mitochondrial boundary membrane contact sites in brain: points of hexokinase and creatine kinase location, and control of Ca2+ transport.

Authors: M Kottke; V Adam; I Riesinger; G Bremm; W Bosch; D Brdiczka; G Sandri; E Panfili
Journal: Biochim Biophys Acta Date: 1988-08-17

5. Inhibition by cyclosporin A of a Ca2+-dependent pore in heart mitochondria activated by inorganic phosphate and oxidative stress.

Authors: M Crompton; H Ellinger; A Costi
Journal: Biochem J Date: 1988-10-01 Impact factor: 3.857

6. The presence of two classes of high-affinity cyclosporin A binding sites in mitochondria. Evidence that the minor component is involved in the opening of an inner-membrane Ca(2+)-dependent pore.

Authors: O McGuinness; N Yafei; A Costi; M Crompton
Journal: Eur J Biochem Date: 1990-12-12

7. Inhibition of Ca2(+)-induced large-amplitude swelling of liver and heart mitochondria by cyclosporin is probably caused by the inhibitor binding to mitochondrial-matrix peptidyl-prolyl cis-trans isomerase and preventing it interacting with the adenine nucleotide translocase.

Authors: A P Halestrap; A M Davidson
Journal: Biochem J Date: 1990-05-15 Impact factor: 3.857

8. Further evidence that cyclosporin A protects mitochondria from calcium overload by inhibiting a matrix peptidyl-prolyl cis-trans isomerase. Implications for the immunosuppressive and toxic effects of cyclosporin.

Authors: E J Griffiths; A P Halestrap
Journal: Biochem J Date: 1991-03-01 Impact factor: 3.857

9. The entrapment of the Ca2+ indicator arsenazo III in the matrix space of rat liver mitochondria by permeabilization and resealing. Na+-dependent and -independent effluxes of Ca2+ in arsenazo III-loaded mitochondria.

Authors: I Al-Nasser; M Crompton
Journal: Biochem J Date: 1986-10-01 Impact factor: 3.857

10. Kinetic evidence for a heart mitochondrial pore activated by Ca2+, inorganic phosphate and oxidative stress. A potential mechanism for mitochondrial dysfunction during cellular Ca2+ overload.

Authors: M Crompton; A Costi
Journal: Eur J Biochem Date: 1988-12-15

65 in total

Review 1. Pathophysiological and protective roles of mitochondrial ion channels.

Authors: B O'Rourke
Journal: J Physiol Date: 2000-11-15 Impact factor: 5.182

2. Biphasic translocation of Bax to mitochondria.

Authors: Michela Capano; Martin Crompton
Journal: Biochem J Date: 2002-10-01 Impact factor: 3.857

3. The relationship between intracellular [Ca(2+)] and Ca(2+) wave characteristics in permeabilised cardiomyocytes from the rabbit.

Authors: C M Loughrey; K E MacEachern; P Neary; G L Smith
Journal: J Physiol Date: 2002-09-15 Impact factor: 5.182

Mitochondrial intermembrane junctional complexes and their role in cell death.

1. A heart mitochondrial Ca2(+)-dependent pore of possible relevance to re-perfusion-induced injury. Evidence that ADP facilitates pore interconversion between the closed and open states.

2. Evidence for the presence of a reversible Ca2+-dependent pore activated by oxidative stress in heart mitochondria.

3. Role of phosphocreatine in energy transport in skeletal muscle of bullfrog studied by 31P-NMR.

4. Mitochondrial boundary membrane contact sites in brain: points of hexokinase and creatine kinase location, and control of Ca2+ transport.

5. Inhibition by cyclosporin A of a Ca2+-dependent pore in heart mitochondria activated by inorganic phosphate and oxidative stress.

6. The presence of two classes of high-affinity cyclosporin A binding sites in mitochondria. Evidence that the minor component is involved in the opening of an inner-membrane Ca(2+)-dependent pore.

7. Inhibition of Ca2(+)-induced large-amplitude swelling of liver and heart mitochondria by cyclosporin is probably caused by the inhibitor binding to mitochondrial-matrix peptidyl-prolyl cis-trans isomerase and preventing it interacting with the adenine nucleotide translocase.

8. Further evidence that cyclosporin A protects mitochondria from calcium overload by inhibiting a matrix peptidyl-prolyl cis-trans isomerase. Implications for the immunosuppressive and toxic effects of cyclosporin.

9. The entrapment of the Ca2+ indicator arsenazo III in the matrix space of rat liver mitochondria by permeabilization and resealing. Na+-dependent and -independent effluxes of Ca2+ in arsenazo III-loaded mitochondria.

10. Kinetic evidence for a heart mitochondrial pore activated by Ca2+, inorganic phosphate and oxidative stress. A potential mechanism for mitochondrial dysfunction during cellular Ca2+ overload.

Review 1. Pathophysiological and protective roles of mitochondrial ion channels.

2. Biphasic translocation of Bax to mitochondria.

3. The relationship between intracellular [Ca(2+)] and Ca(2+) wave characteristics in permeabilised cardiomyocytes from the rabbit.

4. The Arabidopsis cyclophilin gene family.

Review 5. Interplay between mitochondria and cellular calcium signalling.

Review 6. Prerequisites for ubiquinone analogs to prevent mitochondrial permeability transition-induced cell death.

Review 7. Mitochondria: a target for cancer therapy.

Review 8. Mitochondrial medicine: pharmacological targeting of mitochondria in disease.

9. Automated backbone and side-chain assignment of mitochondrial matrix cyclophilin D.

10. Protective effects of hydroxysafflor yellow A on β-amyloid-induced neurotoxicity in PC12 cells.