Oral bioavailability and gender-related pharmacokinetics of celastrol following administration of pure celastrol and its related tablets in rats

Celastrol is a natural compound extracted from the traditional Chinese medicinal herb, Thunder God Vine (TGV). Owing to its potential anti-inflammatory and antitumor effects, celastrol has been considered as a promising candidate for drug development. To establish a sensitive LC–MS/MS method to inve...

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Bibliographic Details
Published in:Journal of ethnopharmacology 2012-10, Vol.144 (1), p.195-200
Main Authors: Zhang, Jun, Li, Chang-Yin, Xu, Mei-juan, Wu, Ting, Chu, Ji-Hong, Liu, Shi-Jia, Ju, Wen-Zheng
Format: Article
Language:English
Subjects:
absorption
Administration, Intravenous
Administration, Oral
Animals
Bioavailability
Biological Availability
Celastrol
computer software
drugs
Female
Gender difference
gender differences
LC–MS/MS
Male
males
medicinal plants
Medicine, Chinese Traditional
oral administration
Pharmacokinetics
Rats
Rats, Sprague-Dawley
Sex Factors
Student's t-test
Tablets
Tripterygium
Triterpenes - administration & dosage
Triterpenes - blood
Triterpenes - pharmacokinetics
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Summary:Celastrol is a natural compound extracted from the traditional Chinese medicinal herb, Thunder God Vine (TGV). Owing to its potential anti-inflammatory and antitumor effects, celastrol has been considered as a promising candidate for drug development. To establish a sensitive LC–MS/MS method to investigate the pharmacokinetic properties of celastrol in rats. Key pharmacokinetic issues of celastrol including oral bioavailability, comparative pharmacokinetics between pure compound and tablet preparation, as well as gender-related pharmacokinetic difference are to be addressed for the first time. Sprague–Dawley rats were administrated an intravenous dose (100μgkg−1) of pure celastrol and an oral dose (1000μgkg−1) of pure celastrol and TGV tablets (corresponding to 534μgkg−1 of celastrol), respectively. At different time points, the concentration of celastrol in rat plasma was determined by a sensitive and well-validated LC–MS/MS method. Main pharmacokinetic parameters including area under the plasma concentration–time curve (AUC), maximal plasma concentration (Cmax), the time for maximal concentration (Tmax) and mean residence time (MRT) were estimated by Drug and Statistic1.0 pharmacokinetic software (Chinese Pharmacological Association, Anhui, PR China). Statistical analysis was performed using two one-side t test with p-values less than 0.05 as the level of significance. The standard curve of celastrol showed good linearity in the concentration range of 0.11∼54.3ngmL−1 in our current method, with acceptable selectivity, precision, recovery, and stability. The oral absolute bioavailability of celastrol significantly increased from 17.06% for pure celastrol to 94.19% for TGV tablets containing equivalent celastrol. After oral administration of TGV tablets, the Cmax and AUC values of celastrol in female rats were (32.03±8.41)μgL−1 and (379.49±118.19)μghL−1, which were significantly higher (p
ISSN:0378-8741
1872-7573
DOI:10.1016/j.jep.2012.09.005