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首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Darunavir and Ritonavir Total and Unbound Plasmatic Concentrations in HIV-HCV-Coinfected Patients with Hepatic Cirrhosis Compared to Those in HIV-Monoinfected Patients
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Darunavir and Ritonavir Total and Unbound Plasmatic Concentrations in HIV-HCV-Coinfected Patients with Hepatic Cirrhosis Compared to Those in HIV-Monoinfected Patients

机译:HIV-HCV合并感染的肝硬化患者的Darunavir和Ritonavir血浆总和未结合血浆浓度与HIV单感染的患者相比

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Our objective was to describe the pharmacokinetic (PK) parameters of total and unbound darunavir and ritonavir concentrations in HIV-hepatitis C virus (HCV)-coinfected patients with cirrhosis, as ritonavir-boosted darunavir is mainly metabolized in the liver, and hepatic cirrhosis might modify darunavir-ritonavir concentrations. This was a prospective, case-control, and unicenter study. HIV-HCV-coinfected patients with compensated cirrhosis (cases) and HIV-monoinfected patients with normal liver function (controls) were included. Darunavir-ritonavir was given at 800/100 mg once daily. Patients were followed for 24 weeks to assess safety and efficacy. A steady-state 12-h PK study was performed. Total and unbound concentrations were determined by liquid chromatography-tandem mass spectrometry. The unbound fraction was obtained by ultrafiltration. The plasma area under the concentration-time curve (AUC) and oral clearance (CL/F) were assessed by noncompartmental models. Thirty patients (20 cases and 10 controls) were included. Among cirrhotic patients, the Child-Pugh score was C in 4 cases, B in 1 case, and A in 15 cases; the median (interquartile range) transient elastography values were 20 kPa (14 to 26 kPa), and 5 patients had prior clinical decompensations. There were no significant differences in the darunavir PK parameters between cases and controls except for longer time to maximum plasma concentrations (Tmax) and half-lives in the cirrhotic patients. There were no significant differences in ritonavir total concentrations, but the unbound concentrations were higher in cirrhotic patients. There were significant correlations between the darunavir total and unbound concentrations in both cirrhotic patients and controls. There were no differences in PK parameters based on Child-Pugh score, liver elasticity, gender, or use of concomitant medications. In conclusion, in HIV-HCV-coinfected patients with clinically compensated cirrhosis receiving darunavir-ritonavir at 800/100 mg once daily, the darunavir total and unbound concentrations are similar to those observed in noncirrhotic patients, and dose adjustments are not necessary.
机译:我们的目的是描述合并了HIV丙型肝炎病毒(HCV)的肝硬化患者的总和未结合的darunavir和ritonavir浓度的药代动力学(PK)参数,因为受ritonavir刺激的darunavir主要在肝脏中代谢,肝硬化可能修改darunavir-ritonavir的浓度。这是一项前瞻性,病例对照和单中心研究。包括HIV-HCV合并感染的肝硬化患者(病例)和HIV单一感染的肝功能正常的患者(对照组)。每天一次,以800/100 mg的剂量给予Darunavir-ritonavir。随访患者24周以评估安全性和有效性。进行了稳态12小时PK研究。通过液相色谱-串联质谱法测定总浓度和未结合浓度。通过超滤获得未结合的级分。通过非房室模型评估浓度-时间曲线(AUC)和口腔清除率(CL / F)下的血浆面积。包括30例患者(20例和10例对照)。在肝硬化患者中,Child-Pugh评分为C 4例,B 1例,A 15例。中位(四分位间距)瞬态弹性成像值是20 kPa(14至26 kPa),并且5例患者先前有临床代偿失调。肝硬化患者的达那那韦PK参数无明显差异,只是达到最大血浆浓度(Tmax)的时间更长和半衰期更长。利托那韦总浓度无明显差异,但肝硬化患者的未结合浓度较高。肝硬化患者和对照组的达那那韦总浓度与未结合浓度之间存在显着相关性。根据Child-Pugh评分,肝弹性,性别或使用辅助药物,PK参数无差异。总之,在接受HIV-HCV感染的临床补偿性肝硬化患者中,每天一次接受darunavir-ritonavir的800/100 mg darunavir-ritonavir的darunavir的总和未结合浓度与在非肝硬化患者中观察到的相似,因此无需调整剂量。

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