Standard name |
GALLUZZI_PREVENT_MITOCHONDIAL_PERMEABILIZATION |
Systematic name |
M7952 |
Brief description |
Proteins acting on mitochondria to prevent membrane permeabilization. |
Full description or abstract |
Mitochondria are vital for cellular bioenergetics and play a central role in determining the point-of-no-return of the apoptotic process. As a consequence, mitochondria exert a dual function in carcinogenesis. Cancer-associated changes in cellular metabolism (the Warburg effect) influence mitochondrial function, and the invalidation of apoptosis is linked to an inhibition of mitochondrial outer membrane permeabilization (MOMP). On theoretical grounds, it is tempting to develop specific therapeutic interventions that target the mitochondrial Achilles' heel, rendering cancer cells metabolically unviable or subverting endogenous MOMP inhibitors. A variety of experimental therapeutic agents can directly target mitochondria, causing apoptosis induction. This applies to a heterogeneous collection of chemically unrelated compounds including positively charged alpha-helical peptides, agents designed to mimic the Bcl-2 homology domain 3 of Bcl-2-like proteins, ampholytic cations, metals and steroid-like compounds. Such MOMP inducers or facilitators can induce apoptosis by themselves (monotherapy) or facilitate apoptosis induction in combination therapies, bypassing chemoresistance against DNA-damaging agents. In addition, it is possible to design molecules that neutralize inhibitor of apoptosis proteins (IAPs) or heat shock protein 70 (HSP70). Such IAP or HSP70 inhibitors can mimic the action of mitochondrion-derived mediators (Smac/DIABLO, that is, second mitochondria-derived activator of caspases/direct inhibitor of apoptosis-binding protein with a low isoelectric point, in the case of IAPs; AIF, that is apoptosis-inducing factor, in the case of HSP70) and exert potent chemosensitizing effects. |
Collection |
C2: Curated CGP: Chemical and Genetic Perturbations |
Source publication |
Pubmed 16892093 Authors: Galluzzi L,Larochette N,Zamzami N,Kroemer G |
Exact source |
Table 2 |
Related gene sets |
(show 1 additional gene sets from the source publication)
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External links |
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Filtered by similarity ?
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Source species |
Homo sapiens |
Contributed by |
Arthur Liberzon (MSigDB Team) |
Source platform or identifier namespace |
HUMAN_GENE_SYMBOL |
Dataset references |
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GTEx compendium
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Global Cancer Map (Broad Institute)
NCI-60 cell lines (National Cancer Institute)
Legacy heatmaps (PNG)
GTEx compendium
Human tissue compendium (Novartis)
Global Cancer Map (Broad Institute)
NCI-60 cell lines (National Cancer Institute)
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Advanced query |
Further investigate
these 14 genes
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Gene families ? |
Categorize these
14 genes by gene family
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Show members |
(show 26 source identifiers mapped to 14 genes)
Source Id |
NCBI (Entrez) Gene Id |
Gene Symbol |
Gene Description |
ADP |
23038 |
WDTC1 |
WD and tetratricopeptide repeats 1 [Source:H... |
ANT |
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ANT1 |
291 |
SLC25A4 |
solute carrier family 25 member 4 [Source:HG... |
ATP |
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Bad |
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Bak |
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Bax |
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Bcl-2 |
596 |
BCL2 |
BCL2 apoptosis regulator [Source:HGNC Symbol... |
Bcl-XL |
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Bcl-w |
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CK |
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HK |
3827 |
KNG1 |
kininogen 1 [Source:HGNC Symbol;Acc:HGNC:6383] |
HKI |
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HKII |
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MUC1 |
4582 |
MUC1 |
mucin 1, cell surface associated [Source:HGN... |
Mcl-1 |
4170 |
MCL1 |
MCL1 apoptosis regulator, BCL2 family member... |
PBR |
706 |
TSPO |
translocator protein [Source:HGNC Symbol;Acc... |
PHGPx |
2879 |
GPX4 |
glutathione peroxidase 4 [Source:HGNC Symbol... |
PKA |
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PKCe |
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PKG |
5592 |
PRKG1 |
protein kinase cGMP-dependent 1 [Source:HGNC... |
SOD2 |
6648 |
SOD2 |
superoxide dismutase 2 [Source:HGNC Symbol;A... |
TXN |
7295 |
TXN |
thioredoxin [Source:HGNC Symbol;Acc:HGNC:12435] |
VDAC1 |
7416 |
VDAC1 |
voltage dependent anion channel 1 [Source:HG... |
VDAC2 |
7417 |
VDAC2 |
voltage dependent anion channel 2 [Source:HG... |
p38 |
1432 |
MAPK14 |
mitogen-activated protein kinase 14 [Source:... |
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Version history |
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