Deubiquitinating Enzymes
Deubiquitinating enzymes (DUBs) are a group of proteases that catalyze the cleavage of protein-ubiquitin bonds. By removing these modifications, DUBs counteract the activity of ubiquitin ligases, which add ubiquitin molecules to target proteins.
Deubiquitinating Enzyme Inhibitors |
|
|---|---|
| Cat. No. | 产品名称/活性 |
| 7845 | AZ1 USP25/28 inhibitor |
| Selective USP25 and USP28 inhibitor | |
| 6776 | G5 |
| Ubiquitin isopeptidase inhibitor; induces apoptosis | |
| 4285 | HBX 41108 |
| Selective USP7 inhibitor | |
| 6718 | ±-MF 094 |
| Selective USP30 inhibitor | |
| 6435 | ML 323 |
| Potent and selective USP1-UAF1 allosteric inhibitor | |
| 4485 | P 22077 |
| USP7 inhibitor | |
| 4482 | PR 619 |
| Broad spectrum DUB inhibitor | |
| 5197 | Spautin 1 |
| USP10 and USP13 inhibitor; inhibits autophagy | |
Other |
|
| Cat. No. | 产品名称/活性 |
| 7280 | GRL 0617 |
| Inhibits deubiquitination activity of SARS-CoV PLpro; displays no inhibition of human DUBs | |
Deubiquitinating enzymes (DUBs) are a group of proteases that catalyze the cleavage of protein-ubiquitin bonds. By removing these modifications, DUBs counteract the activity of ubiquitin ligases, which add ubiquitin molecules to target proteins.
USPs are the largest and best characterized of the DUB family. There are 63 putative human USP genes, and the proteins they encode are normally between 60 and 300 kDa in size. USPs cleave the isopeptide bond at the C-terminus of ubiquitin, preventing proteasomal degradation of specific proteins. By doing so, USPs also maintain a pool of ubiquitin within the cell and help to regulate protein localization and activation.
Deregulation of the ubiquitin-proteasome system (UPS) has been linked to numerous pathologies, including cancer and neurodegeneration; targeting mechanisms upstream of it may constitute an alternative to targeting the proteasome itself, as well as potentially sidestepping acquired resistance to proteasome inhibitors. Consequently, USP inhibitors are undergoing development as cancer therapeutics.
USP7 is particularly well-characterized; it stabilizes both p53 and MDM2, and has an integral role in cell death following DNA damage. Inhibition of USP14 has been shown to enhance resistance to oxidative stress, ostensibly by increasing proteasome activity and degradation of oxidized proteins.
In addition to USPs, other DUBs include UCH, OTU, MJD and JAMM classes. JAMM DUBs are zinc metalloprotease DUBs whereas the remaining groups are classified as cysteine proteases.
External sources of pharmacological information for Deubiquitinating Enzymes :
Deubiquitinating Enzyme Gene Data
| Gene | Species | Gene Symbol | Gene Accession No. | Protein Accession No. |
|---|---|---|---|---|
| Ubiquitin specific peptidase 7 | Human | USP7 | NM_003479 | Q93009 |
| Mouse | Usp7 | NM_001003918 | Q6A4J8 | |
| Rat | Usp7 | NM_001024790 | Q4VSI4 | |
| Ubiquitin specific peptidase 14 | Human | USP14 | NM_005151 | P54578 |
| Mouse | Usp14 | NM_021522 | Q9JMA1 | |
| Rat | Usp14 | NM_001008301 | - | |
| Ubiquitin carboxyl-terminal esterase L1 | Human | UCHL1 | NM_004181 | P09936 |
| Mouse | Uchl1 | NM_011670 | Q9R0P9 | |
| Rat | Uchl1 | NM_017237 | Q00981 |