TY - JOUR
T1 - Pharmacokinetics and Lung Tissue Concentration of Valnemulin in Swine
AU - Zhu, L.X. AU - Zhang, C.Y. AU - Guo, J.P. AU - Zhang, Z. AU - Liu, Y.H. AU - Wang, R. AU - Luo, X.Y.
JO - Journal of Animal and Veterinary Advances
VL - 10
IS - 14
SP - 1824
EP - 1828
PY - 2011
DA - 2001/08/19
SN - 1680-5593
DO - javaa.2011.1824.1828
UR - https://makhillpublications.co/view-article.php?doi=javaa.2011.1824.1828
KW - pig
KW -bioavailability
KW -HPLC-MS/MS
KW -Valnemulin
KW -pharmacokinetic
KW -China
AB - The systemic bioavailability and lung tissue distribution of valnemulin were investigated in swine. About 65 pigs received 10 mg kg-1 body weight of valnemulin by either intravenous (i.v.) or oral (p.o.) route in two studies: study A (10 pigs, i.v. or p.o.) and study B (55 pigs, p.o.). The plasma and lung tissue concentration of the drug were determined by a validated HPLC-MS/MS method. Plasma concentration-time data after i.v. administration (10 mg kg-1 b.w.) were best described by a two-compartment open model. The pharmacokinetic parameters were elimination rate (ke) 0.95±0.17 h-1, the maximum concentrations 4.63±0.66 μg mL-1, area under the plasma concentration-time curve (AUCinf) 5.30±0.37 (h*μg) mL-1. On the other hand, A one-compartment model with a 1st order absorption rate was best fitted to the plasma concentration-time curve of valnemulin after oral administration (10 mg kg-1 b.w.) and the absorption rate (ka) was 0.34±0.03 h-1, the elimination rate (ke) was 1.05±0.19 h-1, the maximum concentration was 0.59±0.08 μg mL-1 at 1.98±0.21 h (tmax), the mean p.o. bioavailability (F) was 57.43%. Following p.o. administration, a mean valnemulin concentration of 0.14 μg g-1 was detected in lung tissue at 36 h postdosing. The lung AUCinf (410.16 h*μg g-1) was 77.39 times higher than the corresponding plasma AUCinf (5.30 h*μg g-1). The apparent elimination half-time for valnemulin in lung was 3.57 h. The advisable bioavailability and extensive distribution to lung tissue following a single dose of valnemulin may be desirable pharmacokinetic attributes for an antimicrobial drug used for the treatment and prevention of respiratory disease in swine.
ER -