PSMB7 Antibody #12197
Inquiry Info. # 12197
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Supporting Data
REACTIVITY | H Mk |
SENSITIVITY | Endogenous |
MW (kDa) | 28 |
SOURCE | Rabbit |
Application Key:
- WB-Western Blotting
Species Cross-Reactivity Key:
- H-Human
- Mk-Monkey
Product Information
Product Usage Information
Application | Dilution |
---|---|
Western Blotting | 1:1000 |
Storage
Protocol
Specificity / Sensitivity
Species Reactivity:
Source / Purification
Background
The core particle performs three types of catalytic activities inside its chamber: chymotrypsin-like, trypsin-like, and caspase-like activities, which are provided by the constitutively expressed PSMB5 (β5/MB1/X/LMPX/Macropain epsilon chain), PSMB7 (β2/Z/Macropain chain Z) and PSMB6 (β1/Y/LMPY/Macropain delta chain) subunits, respectively. These catalytic subunits belong to the N-terminal nucleophile (Ntn) hydrolase family and are characterized by an unusual, essentially single-residue active site: the N-terminal threonine of each proteolytic subunit provides both the catalytic nucleophile (on its side chain) and the primary proton acceptor (on the main chain N-terminus). The catalytic β-subunits are synthesized with N-terminal propeptides, which are removed at the final step of proteasome biogenesis by limited proteolysis to expose the catalytic threonine residues (3). In immune responsive cells the constitutively expressed PSMB6, PSMB7, and PSMB5 subunits are replaced by three highly homologous induced β-subunits: PSMB9 (β1i/LMP2/RING12), PSMB10 (β2i/MECL-1/LMP10), and PSMB8 (β5i/LMP7/RING10), respectively, to form the immunoproteasome that has higher chymotrypsin-like and trypsin-like activities known to be favorable for antigen processing (4,5). Indeed, PSMB7 is downregulated at the protein level by IFN-γ and replaced by PSMB10/MECL-1 in order to remodel the proteolytic specificity of the proteasome for more appropriate immunological processing of endogenous antigens (6). Investigators have shown that PSMB7 expression is upregulated in human colon adenocarcinomas (7). Furthermore, research studies have implicated high expression of PSMB7 as a potential prognostic marker in breast cancer (8).
- Finley, D. (2009) Annu Rev Biochem 78, 477-513.
- Lee, M.J. et al. (2011) Mol Cell Proteomics 10, R110.003871.
- Stringer, J.R. et al. (1977) J Virol 21, 889-901.
- Boes, B. et al. (1994) J Exp Med 179, 901-9.
- Cardozo, C. and Kohanski, R.A. (1998) J Biol Chem 273, 16764-70.
- Hisamatsu, H. et al. (1996) J Exp Med 183, 1807-16.
- Rho, J.H. et al. (2008) J Proteome Res 7, 2959-72.
- Munkácsy, G. et al. (2010) Br J Cancer 102, 361-8.
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