Bcl-xL regulates metabolic efficiency of neurons through interaction with the mitochondrial F1FO ATP synthase

Kambiz N. Alavian,Hongmei Li,Leon P. Collis,Laura Bonanni,Lu Zeng,Silvio Sacchetti,Emma Lazrove,Panah Nabili,Benjamin J. Flaherty,Morven Graham,Yingbei Chen,Shanta M. Messerli,Maria A. Mariggio,Christopher Rahner,Ewan C. McNay,Gordon C. Shore,Peter J. Smith,J. Marie Hardwick,Elizabeth A. Jonas

Bcl-xL regulates metabolic efficiency of neurons through interaction with the mitochondrial F1FO ATP synthase

2011

Kambiz N. Alavian
Hongmei Li
Leon P. Collis
Laura Bonanni
Lu Zeng
Silvio Sacchetti
Emma Lazrove
Panah Nabili
Benjamin J. Flaherty
Morven Graham
Yingbei Chen
Shanta M. Messerli
Maria A. Mariggio
Christopher Rahner
Ewan C. McNay
Gordon C. Shore
Peter J. Smith
J. Marie Hardwick
Elizabeth A. Jonas

ATP production by mitochondria requires the efficient flow of protons through the F1FO ATP-synthase complex. Jonas and colleagues show that Bcl-xL interacts with the F1FO complex in the mitochondrial matrix and increases the efficiency of this enzyme by decreasing proton leak.

Keywords:

Cell biology
Adenosine triphosphate
Mitochondrial Proton-Translocating ATPases
Molecular biology
Bcl-2 Homologous Antagonist-Killer Protein
ATP synthase
Mitochondrial matrix
Biology
ATPase
Mitochondrion
Carbonyl cyanide-p-trifluoromethoxyphenylhydrazone

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

217

Citations