3.4.25.1: proteasome endopeptidase complex
This is an abbreviated version!
For detailed information about proteasome endopeptidase complex, go to the full flat file.
Word Map on EC 3.4.25.1
-
3.4.25.1
-
bortezomib
-
myeloma
-
polyubiquitinated
-
neurodegenerative
-
misfolded
-
lysosomal
-
histone
-
chymotrypsin-like
-
ligases
-
leukemia
-
relapsed
-
nf-kappab
-
immunomodulatory
-
parkinsonism
-
lymphoma
-
deacetylase
-
ubiquitin-dependent
-
alzheimer
-
cyclins
-
hematologic
-
caspase
-
histocompatibility
-
proteostasis
-
ubiquitin-like
-
dexamethasone
-
hsp90
-
deubiquitinating
-
ubiquitin-conjugating
-
calpains
-
autologous
-
inclusions
-
incurable
-
cyclin-dependent
-
short-lived
-
mantle
-
trypsin-like
-
progression-free
-
thalidomide
-
ubiquitin-mediated
-
polyglutamine
-
ikappab
-
mcl-1
-
multisubunit
-
mdm2
-
ikappabalpha
-
parkin
-
rituximab
-
alpha-synuclein
-
single-agent
-
p27kip1
-
synthesis
-
medicine
-
degradation
-
analysis
-
drug development
-
biotechnology
- 3.4.25.1
- bortezomib
- myeloma
-
polyubiquitinated
- neurodegenerative
-
misfolded
- lysosomal
- histone
-
chymotrypsin-like
- ligases
- leukemia
-
relapsed
- nf-kappab
-
immunomodulatory
- parkinsonism
- lymphoma
- deacetylase
-
ubiquitin-dependent
- alzheimer
- cyclins
- hematologic
-
caspase
-
histocompatibility
-
proteostasis
-
ubiquitin-like
- dexamethasone
- hsp90
-
deubiquitinating
-
ubiquitin-conjugating
- calpains
-
autologous
- inclusions
-
incurable
-
cyclin-dependent
-
short-lived
-
mantle
-
trypsin-like
-
progression-free
- thalidomide
-
ubiquitin-mediated
-
polyglutamine
- ikappab
- mcl-1
-
multisubunit
- mdm2
- ikappabalpha
- parkin
- rituximab
- alpha-synuclein
-
single-agent
- p27kip1
- synthesis
- medicine
- degradation
- analysis
- drug development
- biotechnology
Reaction
cleavage of peptide bonds with very broad specificity =
Synonyms
20 S proteasome, 206 proteasome, 20S CP, 20S protease core, 20S proteasome, 26 S proteasome, 26S protease, 26S proteasome, 26S proteasome complex, 27 kDa prosomal protein, 30 kDa prosomal protein, beta1-PF1404, c20S, Component Y8, constitutive proteasome 20S, EC 3.4.22.21, EC 3.4.24.5, EC 3.4.99.46, GPRO-28, HsBPROS26, HSN3, i20S, immunoproteasome 20S, ingensin, KIPase, large multicatalytic protease, macropain, multi-subunit protease complex, multicatalytic endopeptidase complex, Multicatalytic endopeptidase complex C7, multicatalytic protease, multicatalytic proteinase, p27K, PROS-27, PROS-30, PROS-Dm25, PROS-Dm28.1, PROS-Dm29, PROS-Dm35, Pros26.4, prosome, proteasome, proteasome 19S, proteasome 20S, Proteasome component C13, Proteasome component C2, Proteasome component C3, Proteasome component C5, Proteasome component C8, Proteasome component C9, Proteasome component DD4, Proteasome component DD5, Proteasome component pts1, proteasome subunit alpha-type 7-like, PSMA5, Psma8, RING12 protein, RN3, Scl1, SCL1 suppressor protein, SFRICE_003436, T20S, TAS-F22/FAFP98, TAS-G64, TCPR29, tricorn protease, tricorn proteinase, XC3
ECTree
3.4.25.1 proteasome endopeptidase complexAdvanced search results
results (
results (Application
Application on EC 3.4.25.1 - proteasome endopeptidase complex
Please wait a moment until all data is loaded. This message will disappear when all data is loaded.
top
APPLICATION 
ORGANISM
UNIPROT
COMMENTARY 
LITERATURE
analysis
-
simultaneous labeling and detection of constitutive 20S proteasome subunits using an affinity-based probe cocktail and application to biological samples
biotechnology
-
the 20S proteasome could be an as yet not identified bottleneck in the expression and secretion of some heterologous proteins by Streptomyces lividans. Optimization of the production of specific heterologous proteins is likely to require engineered Streptomyces lividans strains, in which the proteasome has been removed
degradation
-
targeted proteasomal knockdown of GFP is induced by use of a specific anti-GFP nanobody in plants. GFP is depleted by a chimeric nanobody fused to a distinct F-box domain, which enables protein degradation via the ubiquitin proteasome pathway
drug development
-
the proteasome is a target for inhibitor development and optimization, overview
medicine
synthesis
-
the incorporation of parus subunits into Arabidopsis holoprotease raises the intriguing possibility that plants synthesize multiple 26S proteasome types with unique properties and/or target specificities
additional information
-
peptide splicing is an intrinsic additional catalytic property of the proteasome, which may provide a qualitative peptide pool for immune selection
medicine
-
nuclear localization of 20S proteasome seems to be associated with the pathogeneses of Parkinson's disease
medicine
-
inhibitor development and optimization of the molecules can lead to better anticancer therapy, overview
medicine
-
Nrf1-mediated proteasome homeostasis can be an attractive target for therapeutic intervention in cancer
medicine
-
Nrf1-mediated proteasome homeostasis can be an attractive target for therapeutic intervention in cancer
medicine
-
proteasome inhibitors and other Hsp70 inducing agents may be useful in the treatment of a variety of genetic diseases caused by missense mutations
medicine
-
proteasome inhibitors are used for the treatment of multiple myeloma and recurring mantle cell lymphoma, e.g. inhibitors MLN9708 and bortezomib, overview
medicine
-
curcumin diminishes DYRK2-mediated 26S proteasome phosphorylation in cells, leading to reduced proteasome activity and impaired cell proliferation. Curcumin synergizes with the therapeutic proteasome inhibitor carfilzomib to induce apoptosis in a variety of proteasome-addicted cancer cells, the drug combination exhibits modest to no cytotoxicity to noncancerous cells. In a breast cancer xenograft model, curcumin treatment significantly reduces tumor burden in immunocompromised mice, showing a similar antitumor effect as CRISPR/Cas9-mediated DYRK2 depletion
