AMPKgamma-1(N-term)(PRKAG1)antibody

AMPKgamma-1(N-term)(PRKAG1)antibody

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上海高创化学科技有限公司

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AMPK gamma-1(N-term)(PRKAG1)antibody
Cat.#: 1569-1
Rabbit Monoclonal Antibody
Clone ID: Y307
Swiss Prot: P54619
Mol Weight: 38kDa
Size: 100ul

Description
The 5-AMP-activated protein kinase (AMPK), a member of the SNF1 (sucrose nonfermentor) kinase family (1), is a heterotrimeric protein comprise of α (63 kDa), β (30 kDa) and γ (38 kDa) subunits. The α subunit is the catalytic subunit, while β and γ are noncatalytic subunits (although they have been found to interact with the active subunit in liver). AMPK regulates fatty acid and sterol synthesis by phosphorylation of acetyl-CoA as well as cholesterol synthesis via phosphorylation and inactivation of hydroxymethylglutaryl-CoA reductase (2). AMPK is activated by AMP and can be also regulated by treatment with purified protein phosphatase in vitro (3).

Recommended Applications
WB, IHC, ICC, IP, FC

Applications and Recommended Dilution Factors
WB: 1:1,000-2,000
IHC: 1:250-500
ICC: 1:50-100
IP: 1:50
FC: 1:100

Species Reactivity
Human

Cross reactivity determined by western blot only.

Products Data 

 


A. Western blot analysis of anti- AMPK gamma-1 (N-term) RabMAb (cat. # 1569-1), dilution 1:2,000. A: Jurkat B: Hela
B. Immunohistochemical analysis of paraffin-embedded human skeletal muscles using anti-AMPK gamma-1 (N-term) RabMAb (cat. # 1569-1).

Specificity
A synthetic peptide corresponding to residues in the N-term of human AMPK gamma-1 subunits was used as an immunogen

Storage Condition and Buffer
Store at -20 °C. Buffer: 50 mM Tris-Glycine (pH 7.4), 0.15 M NaCl, 40% Glycerol, 0.01% sodium azide and 0.05% BSA. Stable for 12 months from date of receipt.

Alternative Names
PRKAG1 antibody, AMPKG antibody, MGC8666 antibody, 5'-AMP-activated protein kinase subunit gamma-1 antibody, antibody

Description References
1. Mitchelhill, K. I., Stapleton, D., Gao, G., House, C., Michell, B., Katsis, F., Witters, L. A., and Kemp, B. E. (1994) J. Biol. Chem. 269, 2361-2364
2. Carling, D., Clarke, P. R., Zammit, V. A., and Hardie, D. G. (1989) Eur. J. Biochem. 186, 129-136
3. Carling, D., Zammit, V. A,, and Hardie, D. G. (1987) FEES Lett. 223,217-222

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