Human 26S Proteasome Protein, CF

Product Discontinued

Human 26S Proteasome Protein, CF Summary

• Details of Functionality: The Human 26S Proteasome can be used for in vitro degradation of appropriate substrates. The Human 26S Proteasome should be used immediately after thawing since it is inherently labile and will dissociate into free 20S and 19S subcomplexes over time. Reaction conditions will need to be optimized for each specific application. We recommend an initial Human 26S Proteasome concentration of 2-20 nM.
• Source: Human embryonic kidney cell, HEK293-derived 26S Proteasome protein
• Protein/Peptide Type: Natural Enzymes
• Purity: >95%, by SDS-PAGE under reducing conditions and visualized by Colloidal Coomassie® Blue stain.

Applications/Dilutions

• Dilutions:
  • Enzyme Activity
• Theoretical MW: 2,100 kDa.
  Disclaimer note: The observed molecular weight of the protein may vary from the listed predicted molecular weight due to post translational modifications, post translation cleavages, relative charges, and other experimental factors.

Packaging, Storage & Formulations

• Storage: Use a manual defrost freezer and avoid repeated freeze-thaw cycles.
  • 12 months from date of receipt, -70 °C as supplied.
  • 3 months, -70 °C under sterile conditions after opening.
• Buffer:

  X mg/ml (X μM) in 20 mM HEPES pH 7.5, 20 mM NaCl, 2 mM Mg-ATP, 15% (v/v) Glycerol

• Purity: >95%, by SDS-PAGE under reducing conditions and visualized by Colloidal Coomassie® Blue stain.

Notes

This product is produced by and ships from R&D Systems, Inc., a Bio-Techne brand.

Alternate Names for Human 26S Proteasome Protein, CF

• 26S Proteasome

Background

The 26S Proteasome is the major non-lysosomal protease in eukaryotic cells and is responsible for the degradation of ubiquitinated substrates and misfolded proteins. It is composed of two subcomplexes: the 20S Proteasome core particle and the 19S Proteasome regulatory particle. The 20S Proteasome facilitates proteolytic cleavage of protein substrates and is composed of 28 subunits arranged into four stacked rings (1,2). The outer rings of the 20S Proteasome are composed of seven related but non-identical, non-catalytic subunits, alpha1-7, that form a gate and restrict substrate access. The inner rings of the 20S Proteasome are composed of seven related but non-identical subunits, beta1-7. Beta1, 2, and 5 have proteyolytic activity. The 19S Proteasome caps one or both ends of the core particle and regulates substrate access to the catalytic core in an ATP-dependent manner by modulating 20S Proteasome conformation (3-5). The 19S Proteasome consists of a base subcomplex and a lid subcomplex. The base subcomplex is composed of six AAA⁺ family members, scaffolding proteins, and regulatory proteins involved in Ubiquitin recognition (2,6). The 19S Proteasome lid subcomplex contains eight subunits plus one deubiquitinating enzyme, Rpn11 (2,6). Small molecules that inhibit the activity of the 26S Proteasome are used to study the function of short-lived intracellular proteins and for the clinical treatment of certain forms of cancer (7). This highly purified 26S Proteasome preparation (from the transformed HEK cell line) can be used in vitro for the degradation of peptide substrates and poly-ubiquitinated proteins.

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14. Hartmann-Peterson R., et al. (2003) Tren.Bioch.Sci 28: 26-318.
15. Kisselev A.F. and Goldberg A.L. (2005) Meth. Enz. 398: 364-3789.
16. Voges D., et al. (1999) Ann. Rev. Biochem. 68: 1015-106810.
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18. Waxman L., et al. (1987) J. Biol. Chem. 262: 2451-2457.

Publications for 26S Proteasome (E-365)(14)

Publications using E-365

• Dubey, AA;Sarkar, A;Milcz, K;Szulc, NA;Thapa, P;Piechota, M;Serwa, RA;Pokrzywa, W; Floxuridine supports UPS independent of germline signaling and proteostasis regulators via involvement of detoxification in C. elegans PLoS genetics 2024-07-31 [PMID: 39083540] (Bioassay, C. elegans)
• M Oro?, M Grochowski, A Jaiswar, J Legierska, K Jastrz?bsk, M Nowak-Niez, M Ko?os, W Ka?miercza, T Olesi?ski, M Lenarcik, M Cybulska, M Mikula, A ?ylicz, M Mi?czy?ska, K Zettl, JR Wi?niewski, D Walerych The molecular network of the proteasome machinery inhibition response is orchestrated by HSP70, revealing vulnerabilities in cancer cells Cell Reports, 2022-09-27;40(13):111428. 2022-09-27 [PMID: 36170818] (Bioassay, Human)
• J Lee, AK Pandey, S Venkatesh, J Thilagavat, T Honda, K Singh, CK Suzuki Inhibition of mitochondrial LonP1 protease by allosteric blockade of ATP -binding and -hydrolysis via CDDO and its derivatives The Journal of Biological Chemistry, 2022-02-11;0(0):101719. 2022-02-11 [PMID: 35151690]
• T Aramburu, J Kelich, C Rice, E Skordalake POT1-TPP1 binding stabilizes POT1, promoting efficient telomere maintenance Computational and structural biotechnology journal, 2022-01-11;20(0):675-684. 2022-01-11 [PMID: 35140887] (Bioassay, Human)
• F Xu, Y Ma, W Huang, J Gao, M Guo, J Li, L Kong, G Liang, R Du, Q Xu, X Wu Typically inhibiting USP14 promotes autophagy in M1-like macrophages and alleviates CLP-induced sepsis Cell Death Dis, 2020-08-20;11(8):666. 2020-08-20 [PMID: 32820146] (Bioassay, Human)
• X Li, Q Huang, H Long, P Zhang, H Su, J Liu A new gold(I) complex-Au(PPh3)PT is a deubiquitinase inhibitor and inhibits tumor growth EBioMedicine, 2018-12-05;0(0):. 2018-12-05 [PMID: 30527624] (Bioassay, Human)
• JH Kim, SK Cho, TR Oh, MY Ryu, SW Yang, WT Kim MPSR1 is a cytoplasmic PQC E3 ligase for eliminating emergent misfolded proteins in Arabidopsis thaliana Proc. Natl. Acad. Sci. U.S.A., 2017-10-30;114(46):E10009-E10017. 2017-10-30 [PMID: 29087340] (Bioassay)
• W Zhou, L Wei, T Xiao, C Lai, M Peng, L Xu, X Luo, S Deng, F Zhang Diabetogenic agent alloxan is a proteasome inhibitor Biochem. Biophys. Res. Commun., 2017-05-11;0(0):. 2017-05-11 [PMID: 28502636] (Bioassay)
• Michal Chojnacki Characterizing polyubiquitinated forms of the neurodegenerative ubiquitin mutant UBB(+1) FEBS Lett, 2016-11-22;590(24):4573-4585. 2016-11-22 [PMID: 27861798] (Bioassay)
• Neerav N Shukla Proteasome addiction defined in Ewing's sarcoma is effectively targeted by a novel class of 19S proteasome inhibitors Cancer Res, 2016-06-02;0(0):. 2016-06-02 [PMID: 27256563] (Bioassay, Human)
• BJ Yang, XX Han, LL Yin, MQ Xing, ZH Xu, HW Xue Arabidopsis PROTEASOME REGULATOR1 is required for auxin-mediated suppression of proteasome activity and regulates auxin signalling Nat Commun, 2016-04-25;7(0):11388. 2016-04-25 [PMID: 27109828] (Enzyme Assay, Human)
• Vallelian F, Deuel J, Opitz L, Schaer C, Puglia M, Lonn M, Engelsberger W, Schauer S, Karnaukhova E, Spahn D, Stocker R, Buehler P, Schaer D Proteasome inhibition and oxidative reactions disrupt cellular homeostasis during heme stress. Cell Death Differ, 2014-10-10;22(4):597-611. 2014-10-10 [PMID: 25301065] (Bioassay)
• Bergamo P, Cocca E, Palumbo R, Gogliettino M, Rossi M, Palmieri G RedOx status, proteasome and APEH: insights into anticancer mechanisms of t10,c12-conjugated linoleic acid isomer on A375 melanoma cells. PLoS ONE, 2013-11-19;8(11):e80900. 2013-11-19 [PMID: 24260504] (Bioassay, Human)
• Sun J, Zhou W, Kaliappan K, Nawaz Z, Slingerland J ERalpha phosphorylation at Y537 by Src triggers E6-AP-ERalpha binding, ERalpha ubiquitylation, promoter occupancy, and target gene expression. Mol Endocrinol, 2012-08-03;26(9):1567-77. 2012-08-03 [PMID: 22865929] (Bioassay, Human)