부산대학교 도서관

Darunavir is effective against wild-type and PI-resistant HIV, and has an oral bioavailability of 37%. It needs to be combined with ritonavir, which increases the bioavailability to 82%. The aim of this study was to evaluate thein-vivoefficacy of the darunavir-SLN and demonstrate lymphatic transport as a contributing pathway in increasing the drug bioavailability. The SLN was prepared by hot-homogenization technique using GMS as lipid.In-vitrodrug release from SLN at the 12th hour was retarded (80.6%) compared to marketed tablet (92.6%).Ex-vivoapparent permeability of the freeze-dried SLN across everted rat intestine was 24 × 10−6at 37 °C and 5.6 × 10−6at 4 °C. The presence of endocytic process inhibitors like chlorpromazine and nystatin reduced it to 18.8 × 10−6and 20.2 × 10−6, respectively, which established involvement of endocytic mechanism in the uptake of SLN.In-vivopharmacokinetic studies on rats demonstrated increase in the AUC of SLN (26) as compared to that of marketed tablet (13.22), while the presence of lymphatic uptake inhibitor cycloheximide lowered the AUC of SLN to 17.19 which further led credence to the involvement of lymphatic uptake behind improved bioavailability. The detection of darunavir in the lymphatic fluid of the rats administered with darunavir-SLN further reinforced the conclusion of SLN being taken up by the lymphatic system. [ABSTRACT FROM AUTHOR]