将福沙普那韦/替诺福韦/恩曲他滨方案中利托那韦的增效剂量从每日一次200毫克降至100毫克之前和之后的稳态安普那韦、替诺福韦和恩曲他滨药代动力学(TELEX II)
Steady-state amprenavir, tenofovir, and emtricitabine pharmacokinetics before and after reducing ritonavir boosting of a fosamprenavir/tenofovir/emtricitabine regimen from 200 mg to 100 mg once daily (TELEX II).
作者信息
Parks David A, Jennings H Clay, Taylor Christopher, Pakes Gary E, Acosta Edward P
机构信息
CentralWest Research, St. Louis, Missouri, USA.
出版信息
HIV Clin Trials. 2009 May-Jun;10(3):160-7. doi: 10.1310/hct1003-160.
PURPOSE
Evaluate how reducing ritonavir (RTV) boosting from 200 mg to 100 mg once daily (QD) affects steady-state pharmacokinetics of components of a fosamprenavir (FPV)-based regimen.
METHODS
Prospective, open-label, pharmacokinetic study in 12 HIV-infected patients stabilized on FPV/RTV 1400 mg/200 mg + tenofovir disoproxil fumarate (TDF)/emtricitabine (FTC) 300 mg/200 mg QD (TELEX II). Pharmacokinetics were assessed by noncompartmental analysis at baseline and 4 weeks after RTV reduction to 100 mg QD.
RESULTS
Baseline median minimum plasma concentration (Cmin) and area under the plasma concentration-time curve over 24 hours post dose (AUC24h) were as follows: APV: 1,708 ng/mL, 84,260 h * ng/mL; tenofovir: 53 ng/mL, 2,420 h * ng/mL; FTC: 58 ng/mL, 9,190 h * ng/mL; RTV: 80 ng/mL, 10,230 h * ng/mL. Four weeks after reducing RTV, changes in Cmin and AUC24h were: APV: +26%, +0.6%; tenofovir: +77%, +30%; FTC: +188%, +13%; RTV -64%, -79%. Component plasma concentration ranges were consistent with historical values. Median APV Cmin was 14.7-fold above the protein-binding-adjusted 50% inhibitory concentration of wild-type HIV. Four weeks after RTV reduction, HIV-1 RNA levels remained <50 copies/mL in all patients, median CD4+ count increased from 465 to 495 cells/mm3, and favorable lipid changes and no adverse events were observed.
CONCLUSION
Reducing RTV boosting from 200 to 100 mg QD of FPV/TDF/FTC QD conferred no detrimental effect on APV, tenofovir, FTC, or RTV pharmacokinetics and maintained virologic suppression.
目的
评估将利托那韦(RTV)的每日剂量从200毫克降至100毫克对基于福沙普那韦(FPV)方案中各成分稳态药代动力学的影响。
方法
对12例稳定接受FPV/RTV 1400毫克/200毫克+替诺福韦酯富马酸盐(TDF)/恩曲他滨(FTC)300毫克/200毫克每日一次(TELEX II)治疗的HIV感染患者进行前瞻性、开放标签的药代动力学研究。在基线以及RTV降至每日100毫克4周后,通过非房室分析评估药代动力学。
结果
基线时血浆最低浓度(Cmin)中位数和给药后24小时血浆浓度 - 时间曲线下面积(AUC24h)如下:阿普那韦(APV):1708纳克/毫升,84260小时·纳克/毫升;替诺福韦:53纳克/毫升,2420小时·纳克/毫升;FTC:58纳克/毫升,9190小时·纳克/毫升;RTV:80纳克/毫升,10230小时·纳克/毫升。RTV降低4周后,Cmin和AUC24h的变化如下:APV:升高26%,升高0.6%;替诺福韦:升高77%,升高30%;FTC:升高188%;升高13%;RTV:降低64%,降低79%。各成分血浆浓度范围与历史值一致。APV的Cmin中位数比野生型HIV经蛋白结合调整后的50%抑制浓度高14.7倍。RTV降低4周后,所有患者的HIV - 1 RNA水平仍<50拷贝/毫升,CD4 + 细胞计数中位数从465个/立方毫米增至495个/立方毫米,且观察到有利的血脂变化且无不良事件发生。
结论
将基于FPV/TDF/FTC每日一次方案中的RTV剂量从200毫克降至100毫克对APV、替诺福韦、FTC或RTV的药代动力学无不利影响,并维持了病毒学抑制。
Zotero 插件