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Query: UMLS:C0002736 (
amyotrophic lateral sclerosis
)
19,048
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
SOD1 is a cause of the fatal, paralytic disorder
ALS
. Although mechanisms underlying mutant SOD1 neurotoxicity remain uncertain, this protein associates with mitochondria. In this issue of Neuron, Israelson et al. show that mutant SOD1 binds and inhibits the mitochondrial channel
VDAC1
. This finding sheds light onto possible molecular links between mutant SOD1, mitochondrial dysfunction, and spinal motor neuron degeneration in inherited
ALS
.
...
PMID:Is amyotrophic lateral sclerosis a mitochondrial channelopathy? 2079 35
Mutations in superoxide dismutase (SOD1) cause
amyotrophic lateral sclerosis
(
ALS
), a neurodegenerative disease characterized by loss of motor neurons. With conformation-specific antibodies, we now demonstrate that misfolded mutant SOD1 binds directly to the voltage-dependent anion channel (
VDAC1
), an integral membrane protein imbedded in the outer mitochondrial membrane. This interaction is found on isolated spinal cord mitochondria and can be reconstituted with purified components in vitro. ADP passage through the outer membrane is diminished in spinal mitochondria from mutant SOD1-expressing
ALS
rats. Direct binding of mutant SOD1 to
VDAC1
inhibits conductance of individual channels when reconstituted in a lipid bilayer. Reduction of
VDAC1
activity with targeted gene disruption is shown to diminish survival by accelerating onset of fatal paralysis in mice expressing the
ALS
-causing mutation SOD1(G37R). Taken together, our results establish a direct link between misfolded mutant SOD1 and mitochondrial dysfunction in this form of inherited
ALS
.
...
PMID:Misfolded mutant SOD1 directly inhibits VDAC1 conductance in a mouse model of inherited ALS. 2079 28
Mutations in superoxide dismutase 1 (SOD1) cause
amyotrophic lateral sclerosis
(
ALS
) in 20% of familial cases (fALS). Mitochondria are one of the targets of mutant SOD1 (mutSOD1) toxicity. We previously demonstrated that at the mitochondria, mutSOD1 forms a toxic complex with Bcl-2, which is then converted into a toxic protein via a structural rearrangement that exposes its toxic BH3 domain (Pedrini et al., 2010). Here we now show that formation of this toxic complex with Bcl-2 is the primary event in mutSOD1-induced mitochondrial dysfunction, inhibiting mitochondrial permeability to ADP and inducing mitochondrial hyperpolarization. In mutSOD1-G93A cells and mice, the newly exposed BH3 domain in Bcl-2 alters the normal interaction between Bcl-2 and
VDAC1
thus reducing permeability of the outer mitochondrial membrane. In motor neuronal cells, the mutSOD1/Bcl-2 complex causes mitochondrial hyperpolarization leading to cell loss. Small SOD1-like therapeutic peptides that specifically block formation of the mutSOD1/Bcl-2 complex, recover both aspects of mitochondrial dysfunction: they prevent mitochondrial hyperpolarization and cell loss as well as restore ADP permeability in mitochondria of symptomatic mutSOD1-G93A mice.
...
PMID:Small peptides against the mutant SOD1/Bcl-2 toxic mitochondrial complex restore mitochondrial function and cell viability in mutant SOD1-mediated ALS. 2384 27
Mutations in superoxide dismutase (SOD1) are the second most common cause of familial
amyotrophic lateral sclerosis
(
ALS
), a fatal neurodegenerative disease caused by the death of motor neurons in the brain and spinal cord. SOD1 neurotoxicity has been attributed to aberrant accumulation of misfolded SOD1, which in its soluble form binds to intracellular organelles, such as mitochondria and ER, disrupting their functions. Here, we demonstrate that mutant SOD1 binds specifically to the N-terminal domain of the voltage-dependent anion channel (
VDAC1
), an outer mitochondrial membrane protein controlling cell energy, metabolic and survival pathways. Mutant SOD1
G93A
and SOD1
G85R
, but not wild type SOD1, directly interact with
VDAC1
and reduce its channel conductance. No such interaction with N-terminal-truncated
VDAC1
occurs. Moreover, a
VDAC1
-derived N-terminal peptide inhibited mutant SOD1-induced toxicity. Incubation of motor neuron-like NSC-34 cells expressing mutant SOD1 or mouse embryonic stem cell-derived motor neurons with different
VDAC1
N-terminal peptides resulted in enhanced cell survival. Taken together, our results establish a direct link between mutant SOD1 toxicity and the
VDAC1
N-terminal domain and suggest that
VDAC1
N-terminal peptides targeting mutant SOD1 provide potential new therapeutic strategies for
ALS
.
...
PMID:A VDAC1-Derived N-Terminal Peptide Inhibits Mutant SOD1-VDAC1 Interactions and Toxicity in the SOD1 Model of ALS. 3147 32
Mitochondria from affected tissues of
amyotrophic lateral sclerosis
(
ALS
) patients show morphological and biochemical abnormalities. Mitochondrial dysfunction causes oxidative damage and the accumulation of ROS, and represents one of the major triggers of selective death of motor neurons in
ALS
. We aimed to assess whether oxidative stress in
ALS
induces post-translational modifications (PTMs) in
VDAC1
, the main protein of the outer mitochondrial membrane and known to interact with SOD1 mutants related to
ALS
. In this work, specific PTMs of the
VDAC1
protein purified by hydroxyapatite from mitochondria of a NSC34 cell line expressing human SOD1G93A, a suitable
ALS
motor neuron model, were analyzed by tryptic and chymotryptic proteolysis and UHPLC/High-Resolution ESI-MS/MS. We found selective deamidations of asparagine and glutamine of
VDAC1
in
ALS
-related NSC34-SOD1G93A cells but not in NSC34-SOD1WT or NSC34 cells. In addition, we identified differences in the over-oxidation of methionine and cysteines between
VDAC1
purified from
ALS
model or non-
ALS
NSC34 cells. The specific range of PTMs identified exclusively in
VDAC1
from NSC34-SOD1G93A cells but not from NSC34 control lines, suggests the appearance of important changes to the structure of the
VDAC1
channel and therefore to the bioenergetics metabolism of
ALS
motor neurons. Data are available via ProteomeXchange with identifier <PXD022598>.
...
PMID:Post-Translational Modification Analysis of VDAC1 in ALS-SOD1 Model Cells Reveals Specific Asparagine and Glutamine Deamidation. 3327 91
