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Pharmacokinetics of low-dose lopinavir/ritonavir tablet formulation in HIV-1 infected children

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dc.contributor.author Thanyawee Puthanakit
dc.contributor.author Kiat Ruxrungtham
dc.contributor.author Chitsanu Pancharoen
dc.contributor.author Jintanat Ananworanich
dc.contributor.author Torsak Burunupradah
dc.contributor.author Arunee Klinklom
dc.contributor.other Chulalongkorn University. Faculty of Medicine
dc.date.accessioned 2018-04-27T08:36:41Z
dc.date.available 2018-04-27T08:36:41Z
dc.date.issued 2010
dc.identifier.uri http://cuir.car.chula.ac.th/handle/123456789/58579
dc.description.abstract Methods: This was an open-label, cross-over study of 24 HIV-infected children with HIV RNA < 50 copies/ml comparing PK parameter of standard dose LPV/r and low dose of LPV/r for 4 weeks. LPV dosage was prescribed by body weight band; 25~35 kg: LPV/r 300/75 vs. 200/50 mg, > 35 kg 400/100 vs. 300/75 mg. Glood samples were drawn at 0 (pre-dose), 2,4,6,8, 10 and 12 hours. Plasma concentrations of LPV and RTV were measured by HPLC method. The acceptable C12h is > 1 mg/L. The HIV RNA was measured at week 12 after switch back to standard dose for 4 weeks. Results: Twenty four children were included. Median (interquartile range) age, body weight, 3 CD4 count were 13.5 (12-15) years, 33.4 (28.3-41.1) kg, 913(737-1,178) ce"sl mrn . Geometric mean (95% Confidence I nterval) value with standard dose lopinavir AUCo.12 h' C max ,C 12h and T half were 93.8 (82.9-106.3) mg.h/L, 10.8(9.6-12.0) mg/L, 3.7(3.0-4.6) mg/L, and 4.8 (4.0-5.8) h respectively. For low dose LPV these values were 83.1 (72.2-95.6) mg .h/l, 10.7 (9.5-12.0) mg/L, 2.8 (2.1-3.6) mg/L, and 4.1 (3.5-4.8) h, respectively. In the multivariate analysis, there was no significant different in LPV AUC (p=0.35) and C12h (p=0.65) between standard and low dose LPV. But the AUC of ritonavir is the strong predictor for LPV AUC and C12h (p<0.001). One child (3%) had C12h < 1 mg/L (0.82 mg/L) but still had undetectable HIV RNA. There were 2 children had HIV RNA = 52 and 99 copies/ml but C12h >1 mg/L. Conclusions: Low dose of LPV/r provide adequate pharmacokinetic parameters. Successful usage of low dose LPV/r could have a significant public health impact in reducing side effects and costs related to treating complications and procuring the drug. A larger randomized clinical study to assess efficecy of low dose vs. standard dose of LPV/r among HIV-infected children should be explored. en_US
dc.description.sponsorship This research is supported by Rachadapiseksompotch Endowment Fund, Chulalongkorn University in Year 2010 en_US
dc.language.iso en en_US
dc.publisher Chulalongkorn University en_US
dc.rights Chulalongkorn University en_US
dc.subject Pharmacokinetics en_US
dc.subject HIV-positive children en_US
dc.subject HIV (Viruses) en_US
dc.subject Lopinavir en_US
dc.subject Ritonavir en_US
dc.subject Antiviral agents en_US
dc.title Pharmacokinetics of low-dose lopinavir/ritonavir tablet formulation in HIV-1 infected children en_US
dc.title.alternative โครงการวิจัยเพื่อศึกษาเปรียบเทียบเภสัชจลนศาสตร์ ระหว่างการใช้ยาต้านไวรัสโลฟินาเวียร์/ริโทนาเวียร์ชนิดเม็ดในขนาดมาตรฐานและขนาดต่ำในเด็กติดเชื้อเอชไอวี en_US
dc.type Technical Report en_US
dc.email.author Thanyawee.P@chula.ac.th
dc.email.author kiat.r@chula.ac.th
dc.email.author Chitsanu.P@Chula.ac.th
dc.email.author No information provided
dc.email.author No information provided
dc.email.author No information provided


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