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Catalog: | HY-12942 |
Brand: | MCE |
CAS: | 1301214-47-0 |
MDL | MFCD28502250 |
---|---|
Molecular Weight | 405.49 |
Molecular Formula | C23H27N5O2 |
SMILES | O=C1CC2(CCN(C(C3=CC=C4C(NC(C)=N4)=C3)=O)CC2)CC5=C1N(C(C)C)N=C5 |
PF-05175157 is broad spectrum acetyl-CoA carboxylase ( ACC ) inhibitor with IC 50 s of 27.0, 33.0, 23.5 and 50.4 nM for ACC1 (human), ACC2 (human), ACC1 (rat), ACC2 (rat), respectively.
IC50: 27.0 nM (ACC1 (human)), 33.0 nM (ACC2 (human)), 23.5 nM (ACC1 (rat)), 50.4 nM (ACC2 (rat)) [1]
PF-05175157 is broad spectrum acetyl-CoA carboxylase (ACC) inhibitor with IC 50 s of 27.0±2.7, 33.0±4.1, 23.5±1.1 and 50.4±2.6 nM for ACC1 (human), ACC2 (human), ACC1 (rat) and ACC2 (rat), respectively. The in vitro metabolism of PF-05175157 (Compound 9) is evaluated in microsomes from rat, dog, and human hepatocytes. PF-05175157 is not metabolized in rat, dog, or human microsomes. PF-05175157 is also stable in human hepatocyte incubations, but is minimally metabolized by recombinant human CYP3A4 and CYP3A5. PF-05175157 inhibits formation of malonyl-CoA in a concentration-dependent manner with a potency (EC 50 =30 nM) in rat hepatocytes consistent with its potency against rat ACC1 (24 nM) [1] .
MCE has not independently confirmed the accuracy of these methods. They are for reference only.
Oral administration (3 mg/kg) to rats and dogs show bioavailability of 40% and 54%, respectively, consistent with the low microsomal clearance and good solubility at low pH. Formation of the direct product of ACC, malonyl-CoA, in the skeletal muscle and liver of lean rats is assessed 1 h following an acute oral dose of PF-05175157, showing concentration-dependent reductions in both skeletal muscle and liver malonyl-CoA. At the nadir, quadriceps and liver malonyl-CoA levels are reduced by 76% and 89%, respectively. The EC 50 s for inhibition of quadriceps and liver malonyl-CoA are 870 and 540 nM, respectively, determined from unbind plasma concentrations of PF-05175157. Acute oral administration of PF-05175157 inhibits hepatic DNL in rats in an unbind plasma drug concentration-dependent manner. PF-05175157 inhibits up to 82% of the incorporation of [ 14 C]acetate into [ 14 C]lipids with an EC 50 of 326 nM [1] .
MCE has not independently confirmed the accuracy of these methods. They are for reference only.
NCT Number | Sponsor | Condition | Start Date | Phase |
---|---|---|---|---|
NCT02100527 | Pfizer |
Acne Vulgaris
|
April 2014 | Phase 2 |
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Healthy
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March 2013 | Phase 1 |
NCT02053116 | Pfizer |
Type 2 Diabetes Mellitus
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March 2014 | Phase 2 |
NCT01757756 | Pfizer |
Diabetes Mellitus|Diabetes Mellitus, Type 2|Glucose Metabolism Disorders
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October 2012 | Phase 1 |
NCT01433380 | Pfizer |
Diabetes Mellitus, Type 2
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July 2011 | Phase 1 |
NCT02053103 | Pfizer |
Type 2 Diabetes Mellitus
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March 2014 | Phase 2 |
NCT01274663 | Pfizer |
Diabetes Mellitus, Type 2
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November 2010 | Phase 1 |
NCT01792635 | Pfizer |
Diabetes Mellitus, Type 2
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December 2012 | Phase 2 |
NCT01819922 | Pfizer |
Healthy
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April 2013 | Phase 1 |
NCT01469468 | Pfizer |
Type 2 Diabetes Mellitus
|
November 2011 | Phase 1 |
NCT01807377 | Pfizer |
Diabetes Mellitus Type 2
|
April 2013 | Phase 1 |
NCT01396161 | Pfizer |
Diabetes Mellitus, Type 2
|
July 2011 | Phase 1 |
NCT01537497 | Pfizer |
Diabetes Mellitus, Type 2
|
March 2012 | Phase 1 |
Solid
Room temperature in continental US; may vary elsewhere.
Powder | -20°C | 3 years |
---|---|---|
4°C | 2 years | |
In solvent | -80°C | 6 months |
-20°C | 1 month |
DMSO : 30 mg/mL ( 73.98 mM ; Need ultrasonic and warming)
Concentration Solvent Mass | 1 mg | 5 mg | 10 mg |
---|
1 mM | 2.4662 mL | 12.3308 mL | 24.6615 mL |
5 mM | 0.4932 mL | 2.4662 mL | 4.9323 mL |
10 mM | 0.2466 mL | 1.2331 mL | 2.4662 mL |
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