Product Details
Place of Origin: China
Brand Name: Sunshine
Certification: ISO,COA
Model Number: 73963-72-1
Payment & Shipping Terms
Minimum Order Quantity: Negotiation
Price: Negotiation
Packaging Details: Bag,Drum
Delivery Time: 7-15 days
Payment Terms: L/C, D/A, T/T, Western Union
Supply Ability: TON
CAS NO:: |
73963-72-1 |
Appearance:: |
Off-white Solid |
Molecular Formula:: |
C20H27N5O2 |
Molecular Weight:: |
369.46100 |
EINECS NO:: |
689-122-9 |
MDL NO:: |
MFCD00866780 |
CAS NO:: |
73963-72-1 |
Appearance:: |
Off-white Solid |
Molecular Formula:: |
C20H27N5O2 |
Molecular Weight:: |
369.46100 |
EINECS NO:: |
689-122-9 |
MDL NO:: |
MFCD00866780 |
Product Description:
Product Name: Cilostazol CAS NO: 73963-72-1
Synonyms:
6-[4-(1-cyclohexyl-1h-tetrazol-5-yl)butoxy]-3,4-dihydro-2(1h)-quinolinone additional name: 6-[4-(1-cyclohexyl-5-tetrazolyl)butoxy]-1,2,3,4- tetrahydro-2-oxoquinolinone;
OPC-13013, Pletal, 6-[4-(1-Cyclohexyl-1H-tetrazol-5-yl)butoxy]-3,4-dihydro-2(1H)-quinolinone;
Chemical & Physical Properties:
Appearance: Off-white solid
Assay :≥99.00%
Density: 1.34 g/cm3
Boiling Point: 664.7℃ at 760 mmHg
Melting Point: 159-160℃
Flash Point: 355.8℃
Refractive Index: 1.675
Storage Condition: Store in original container in a cool dark place.
Safety Information:
RTECS: VC8277500
HS Code: 2933990090
WGK Germany: 2
Hazard Code: Xi
A potent phosphodiesterase III A (PDE3A) inhibitor (IC50=0.2uM) and inhibitor of adenosine uptake. Has antimitogeni, antithrombotic, vasodilatory and cardiotonic properties in vivo. Also affects lipid levels in vivo. Cilostazol(OPC 13013; OPC 21) is a potent inhibitor of PDE3A, the isoform of PDE 3 in the cardiovascular system (IC50=0.2 uM).IC50 Value: 0.2 uM Target: PDE3Ain vitro: Cilostazol caused a concentration-dependent increase in the cAMP level in rabbit and human platelets with similar potency. Furthermore, cilostazol and milrinone were equally effective in inhibiting human platelet aggregation with a median inhibitory concentration (IC50) of 0.9 and 2 microM, respectively. In rabbit ventricular myocytes, however, cilostazol elevated cAMP levels to a significantly lesser extent (p < 0.05 vs. milrinone). Cilostazol inhibited SIPA dose-dependently in vitro. The IC50 value of cilostazol for inhibition of SIPA was 15 +/- 2.6 microM (m +/- SE, n=5), which was very similar to that (12.5 +/- 2.1 microM) for inhibition of ADP-induced platelet aggregation. Cilostazolpotentiates the inhibition of SIPA by PGE1 and enhances its ability to increase cAMP concentrations [3].in vivo: A single oral adminstration of 100 mgcilostazol to healthy volunteers produced a significant inhibition of SIPA. Male C57BL/6J mice were assigned to five groups: mice fed a normal diet (groups 1 and 2); 0.1% or 0.3% cilostazol-containing diet (groups 3 and 4, respectively); and 0.125% clopidogrel-containing diet (group 5). Two weeks after feeding, groups 2-5 were intraperitoneally administered carbon tetrachloride (CCl4 ) twice a week for 6 weeks, while group 1 was treated with the vehicle alone .Toxicity: Cilostazol in addition to dual antiplatelet therapy appears to be effective in reducing the risk of restenosis and repeat revascularization after PCI without any significant benefits for mortality or stent thrombosis.
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