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Formula | C21H22ClN3O3 |
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Molecular Weight | 399.87 | CAS No. | 186392-40-5 | ||||||||
Solubility (25°C)* | In vitro | DMSO | 80 mg/mL (200.06 mM) | ||||||||
Water | Insoluble | ||||||||||
Ethanol | Insoluble | ||||||||||
In vivo (Add solvents to the product individually and in order) |
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* <1 mg/ml means slightly soluble or insoluble. * Please note that Selleck tests the solubility of all compounds in-house, and the actual solubility may differ slightly from published values. This is normal and is due to slight batch-to-batch variations. * Room temperature shipping (Stability testing shows this product can be shipped without any cooling measures.) |
Description | CP-91149 is a selective glycogen phosphorylase (GP) inhibitor with IC50 of 0.13 μM in the presence of glucose, 5- to 10-fold less potent in the absence of glucose. | ||
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In vitro | CP-91149 displays 200-fold higher inhibitory activity against human liver glycogen phosphorylase a (HLGPa) than caffeine (IC50 = 26 μM). CP-91149 (10-100 μM) inhibits -stimulated glycogenolysis in isolated rat hepatocytes in a dose-dependent manner, and in primary human hepatocytes with IC50 of ~2.1 μM. [1] CP-91149 also potently inhibits the activities of human muscle phosphorylase a and b with IC50 of 0.2 μM and ~0.3 μM, respectively. CP-91149 treatment at 2.5 μM induces inactivation of phosphorylase and sequential activation of glycogen synthase in hepatocytes, and increases glycogen synthesis by 7-fold at 5 mM glucose and by 2-fold at 20 mM glucose. CP-91149 can partially counteract the effects of phosphorylase overexpression. [2] CP-91149 also potently inhibits brain GP with IC50 of 0.5 μM in A549 cells. CP-91149 treatment at 10-30 μM causes significant glycogen accumulation in A549 and HSF55 cells. CP-91149 treatment increases G1-phase cells with a significant reduction of the S-phase population in HSF55 cells, correlated with increased expression of p21 and p27. [3] CP-91149 also promotes the dephosphorylation and activation of GS (glycogen synthase) in non-engineered or GP-overexpressing cultured human muscle cells, but exclusively in glucose-deprived cells. [4] |
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In vivo | Oral administration of CP-91149 to diabetic ob/ob mice at 25-50 mg/kg causes rapid (3 hours) glucose lowering by 100-120 mg/dl without producing hypoglycemia, resulting from inhibition of glycogenolysis in vivo. CP-91149 treatment does not lower glucose levels in normoglycemic, nondiabetic mice. [1] In the non-fasted Goto-Kakizaki (GK) rats, administration of CP-91149 in combination with CS-917 suppresses hepatic glycogen reduction by CS-917 and decreases plasma glucose more than single administration of CS-917. [5] |
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, , Mol Cancer Res, 2014, 12(11):1547-59.
Regulation of stress granule formation in human oligodendrocytes [ Nat Commun, 2024, 15(1):1524] | PubMed: 38374028 |
Glycogenesis and glyconeogenesis from glutamine, lactate and glycerol support human macrophage functions [ EMBO Rep, 2024, 10.1038/s44319-024-00278-4] | PubMed: 39424955 |
Mutant IDH regulates glycogen metabolism from early cartilage development to malignant chondrosarcoma formation [ Cell Rep, 2023, 42(6):112578] | PubMed: 37267108 |
Intracellular energy controls dynamics of stress-induced ribonucleoprotein granules [ Nat Commun, 2022, 13(1):5584] | PubMed: 36151083 |
Intracellular energy controls dynamics of stress-induced ribonucleoprotein granules [ Nat Commun, 2022, 13(1):5584] | PubMed: 36151083 |
TCR activation directly stimulates PYGB-dependent glycogenolysis to fuel the early recall response in CD8+ memory T cells [ Mol Cell, 2022, S1097-2765(22)00538-X] | PubMed: 35738262 |
A genome-wide CRISPR-Cas9 screen identifies CENPJ as a host regulator of altered microtubule organization during Plasmodium liver infection [ Cell Chem Biol, 2022, S2451-9456(22)00205-7] | PubMed: 35738280 |
Analysis of the expression, function and signaling of glycogen phosphorylase isoforms in hepatocellular carcinoma [ Oncol Lett, 2022, 24(2):244] | PubMed: 35761940 |
Glycogen Metabolism Supports Early Glycolytic Reprogramming and Activation in Dendritic Cells in Response to Both TLR and Syk-Dependent CLR Agonists. [ Cells, 2020, 9(3)] | PubMed: 32183271 |
Glycogen Metabolism Supports Early Glycolytic Reprogramming and Activation in Dendritic Cells in Response to Both TLR and Syk-Dependent CLR Agonists [ Cells, 2020, 9(3)E715] | PubMed: 32183271 |
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