Difference between revisions of "Rostovtseva 2008 Proc Natl Acad Sci U S A"
Harrison DK (talk | contribs) |
|||
| Line 4: | Line 4: | ||
|authors=Rostovtseva TK, Sheldon KL, Hassanzadeh E, Monge C, Saks V, Bezrukov SM, Sackett DL | |authors=Rostovtseva TK, Sheldon KL, Hassanzadeh E, Monge C, Saks V, Bezrukov SM, Sackett DL | ||
|year=2008 | |year=2008 | ||
|journal=Proc | |journal=Proc Natl Acad Sci U S A | ||
|abstract=Regulation of mitochondrial outer membrane (MOM) permeability | |abstract=Regulation of mitochondrial outer membrane (MOM) permeability has dual importance: in normal metabolite and energy exchange between mitochondria and cytoplasm and thus in control of respiration, and in apoptosis by release of apoptogenic factors into the cytosol. However, the mechanism of this regulation, dependent on the voltage-dependent anion channel (VDAC), the major channel of MOM, remains controversial. A long-standing puzzle is that in permeabilized cells, adenine nucleotide translocase (ANT) is less accessible to cytosolic ADP than in isolated mitochondria. We solve this puzzle by finding a missing player in the regulation of MOM permeability: the cytoskeletal protein tubulin. We show that nanomolar concentrations of dimeric tubulin induce voltage-sensitive reversible closure of VDAC reconstituted into planar phospholipid membranes. Tubulin strikingly increases VDAC voltage sensitivity and at physiological salt conditions could induce VDAC closure at <10 mV transmembrane potentials. Experiments with isolated mitochondria confirm these findings. Tubulin added to isolated mitochondria decreases ADP availability to ANT, partially restoring the low MOM permeability (high apparent Km for ADP) found in permeabilized cells. Our findings suggest a previously unknown mechanism of regulation of mitochondrial energetics, governed by VDAC and tubulin at the mitochondria–cytosol interface. This tubulin–VDAC interaction requires tubulin anionic C-terminal tail (CTT) peptides. The significance of this interaction may be reflected in the evolutionary conservation of length and anionic charge in CTT throughout eukaryotes, despite wide changes in the exact sequence. Additionally, tubulins that have lost significant length or anionic character are only found in cells that do not have mitochondria. | ||
has dual importance: in normal metabolite and energy exchange | |||
between mitochondria and cytoplasm and thus in control of respiration, | |||
and in apoptosis by release of apoptogenic factors into the | |||
cytosol. However, the mechanism of this regulation, dependent on | |||
the voltage-dependent anion channel (VDAC), the major channel of | |||
MOM, remains controversial. A long-standing puzzle is that in permeabilized | |||
cells, adenine nucleotide translocase (ANT) is less accessible | |||
to cytosolic ADP than in isolated mitochondria. We solve this | |||
puzzle by finding a missing player in the regulation of MOM permeability: | |||
the cytoskeletal protein tubulin. We show that nanomolar | |||
concentrations of dimeric tubulin induce voltage-sensitive reversible | |||
closure of VDAC reconstituted into planar phospholipid membranes. | |||
Tubulin strikingly increases VDAC voltage sensitivity and at physiological | |||
salt conditions could induce VDAC closure at <10 mV transmembrane | |||
potentials. Experiments with isolated mitochondria confirm these | |||
findings. Tubulin added to isolated mitochondria decreases | |||
ADP availability to ANT, partially restoring the low MOM permeability | |||
(high apparent Km for ADP) found in permeabilized cells. Our findings | |||
suggest a previously unknown mechanism of regulation of mitochondrial | |||
energetics, governed by VDAC and tubulin at the | |||
anionic C-terminal tail (CTT) peptides. The significance of this interaction | |||
may be reflected in the evolutionary conservation of length | |||
and anionic charge in CTT throughout eukaryotes, despite wide | |||
changes in the exact sequence. Additionally, tubulins that have lost | |||
significant length or anionic character are only found in cells that do | |||
not have mitochondria. | |||
|keywords=Evolution, Microtubules, Oxidative phosphorylation, VDAC, Tubulin C-terminal | |keywords=Evolution, Microtubules, Oxidative phosphorylation, VDAC, Tubulin C-terminal | ||
|mipnetlab=EE_Tallinn_Saks VA, FR_Grenoble_Saks VA | |mipnetlab=EE_Tallinn_Saks VA, FR_Grenoble_Saks VA | ||
| Line 40: | Line 13: | ||
|instruments=Oxygraph-2k | |instruments=Oxygraph-2k | ||
|organism=Rat | |organism=Rat | ||
|tissues=Cardiac | |tissues=Cardiac muscle, Neurons; Brain | ||
|preparations=Isolated Mitochondria | |preparations=Isolated Mitochondria | ||
|topics=Coupling; Membrane Potential | |topics=Coupling; Membrane Potential | ||
|discipline=Mitochondrial Physiology, Biomedicine | |discipline=Mitochondrial Physiology, Biomedicine | ||
}} | }} | ||
Revision as of 07:19, 5 April 2012
| Rostovtseva TK, Sheldon KL, Hassanzadeh E, Monge C, Saks V, Bezrukov SM, Sackett DL (2008) Tubulin binding blocks mitochondrial voltage-dependent anion channel and regulates respiration. Proc Natl Acad Sci USA 105: 18746-18751. |
Rostovtseva TK, Sheldon KL, Hassanzadeh E, Monge C, Saks V, Bezrukov SM, Sackett DL (2008) Proc Natl Acad Sci U S A
Abstract: Regulation of mitochondrial outer membrane (MOM) permeability has dual importance: in normal metabolite and energy exchange between mitochondria and cytoplasm and thus in control of respiration, and in apoptosis by release of apoptogenic factors into the cytosol. However, the mechanism of this regulation, dependent on the voltage-dependent anion channel (VDAC), the major channel of MOM, remains controversial. A long-standing puzzle is that in permeabilized cells, adenine nucleotide translocase (ANT) is less accessible to cytosolic ADP than in isolated mitochondria. We solve this puzzle by finding a missing player in the regulation of MOM permeability: the cytoskeletal protein tubulin. We show that nanomolar concentrations of dimeric tubulin induce voltage-sensitive reversible closure of VDAC reconstituted into planar phospholipid membranes. Tubulin strikingly increases VDAC voltage sensitivity and at physiological salt conditions could induce VDAC closure at <10 mV transmembrane potentials. Experiments with isolated mitochondria confirm these findings. Tubulin added to isolated mitochondria decreases ADP availability to ANT, partially restoring the low MOM permeability (high apparent Km for ADP) found in permeabilized cells. Our findings suggest a previously unknown mechanism of regulation of mitochondrial energetics, governed by VDAC and tubulin at the mitochondria–cytosol interface. This tubulin–VDAC interaction requires tubulin anionic C-terminal tail (CTT) peptides. The significance of this interaction may be reflected in the evolutionary conservation of length and anionic charge in CTT throughout eukaryotes, despite wide changes in the exact sequence. Additionally, tubulins that have lost significant length or anionic character are only found in cells that do not have mitochondria. • Keywords: Evolution, Microtubules, Oxidative phosphorylation, VDAC, Tubulin C-terminal
• O2k-Network Lab: EE_Tallinn_Saks VA, FR_Grenoble_Saks VA
Labels:
Organism: Rat
Tissue;cell: Cardiac muscle"Cardiac muscle" is not in the list (Heart, Skeletal muscle, Nervous system, Liver, Kidney, Lung;gill, Islet cell;pancreas;thymus, Endothelial;epithelial;mesothelial cell, Blood cells, Fat, ...) of allowed values for the "Tissue and cell" property., Neurons; Brain"Neurons; Brain" is not in the list (Heart, Skeletal muscle, Nervous system, Liver, Kidney, Lung;gill, Islet cell;pancreas;thymus, Endothelial;epithelial;mesothelial cell, Blood cells, Fat, ...) of allowed values for the "Tissue and cell" property.
Preparation: Isolated Mitochondria"Isolated Mitochondria" is not in the list (Intact organism, Intact organ, Permeabilized cells, Permeabilized tissue, Homogenate, Isolated mitochondria, SMP, Chloroplasts, Enzyme, Oxidase;biochemical oxidation, ...) of allowed values for the "Preparation" property.
Regulation: Coupling; Membrane Potential"Coupling; Membrane Potential" is not in the list (Aerobic glycolysis, ADP, ATP, ATP production, AMP, Calcium, Coupling efficiency;uncoupling, Cyt c, Flux control, Inhibitor, ...) of allowed values for the "Respiration and regulation" property.
HRR: Oxygraph-2k
