product name Fexofenadine HCl
Description: Fexofenadine (also known as MDL 16455A) is an potent inhibitor of histamine H1 receptor. Fexofenadine exhibits a potent and concentration-dependent anti-anaphylactic activity with an IC50 value of 95.5nM. Fexofenadine shows only a weak competitive antagonist behaviour for the 5-HT2A receptorsfrom rat caudal artery with pA2 of 5.2. The IC50 of verapamil is 8.44 mM on the P-gp-mediated secretion of Fexofenadine.
References: Drugs R D. 2005;6(6):371-84; J Pharm Sci. 2005 Feb;94(2):233-9.
538.12
Formula
C32H39NO4.HCl
CAS No.
153439-40-8
Storage
-20℃ for 3 years in powder form
-80℃ for 2 years in solvent
Solubility (In vitro)
DMSO: 107 mg/mL (198.8 mM)
Water: 2 mg/mL (3.7 mM)
Ethanol: 107 mg/mL (198.8 mM)
Solubility (In vivo)
Synonyms
MDL 16455A
other peoduct :References PubMed ID::http://www.ncbi.nlm.nih.gov/pubmed/19427028
| In Vitro |
In vitro activity: Fexofenadine exhibits a potent and concentration-dependent anti-anaphylactic activity with an IC50 value of 95.5nM. Fexofenadine shows only a weak competitive antagonist behaviour for the 5-HT2A receptorsfrom rat caudal artery with pA2 of 5.2. All four P-gp inhibitors has a strong, concentration-dependent effect on the Papp of fexofenadine in both directions in the Caco-2 cell model. The IC50 of verapamil is 8.44 mM on the P-gp-mediated secretion of Fexofenadine. Fexofenadine causes a significant increase in the QT and Tp-e intervals and receives a significant TdP score at doses greater than 100 fold its free TPC in the rabbit left ventricular wedge preparation. Kinase Assay: Cell Assay: |
|---|---|
| In Vivo | Fexofenadine is excreted unchanged in the urine, bile, and gastrointestinal tract, indicating minimal metabolism in rats, making it an ideal probe to study transport processes. Coadministration of Fexofenadine with Ketoconazole increases the oral exposure of Fexofenadine by 187% in rats. In contrast, coadministration of Fexofenadine with orange juice or apple juice to rats decreases the oral exposure of Fexofenadine by 31% and 22%, respectively. Increasing the quantity of orange or apple juice administered further decreases the oral exposure of Fexofenadine, by 40% and 28%, respectively. Biliary excretion clearance of Fexofenadine (17 ml/min/kg) accounts for almost 60% of the total body clearance (30 ml/min/kg) in mice. Knockout mice of Mdr1a/1b P-gp does not affect the biliary excretion clearance with regard to both plasma and liver concentrations, whereas the absence of P-gp causes a 6-fold increase in the plasma concentration and 3-fold higher brain-to-plasma concentration ratio after oral administration. |
| Animal model | |
| Formulation & Dosage | |
| References | Drugs R D. 2005;6(6):371-84; J Pharm Sci. 2005 Feb;94(2):233-9. |
