Patel Nimish, Nasiri Mona, Koroglu Arden, Amin Ronish, McGuey Liam, McNutt Louise-Anne, Roman Martha, Miller Christopher
1 Albany College of Pharmacy and Health Sciences , Albany, New York.
AIDS Res Hum Retroviruses. 2015 Feb;31(2):189-97. doi: 10.1089/AID.2014.0215. Epub 2015 Jan 6.
The objectives were to (1) compare the frequency of contraindicated drug-drug interactions (XDDI) when simeprevir (SIM)- and sofosbuvir (SOF)-containing regimens are theoretically added to a patient's medication profile; (2) identify which hepatitis C (HCV) regimen is associated with the lowest frequency of XDDIs within different types of antiretroviral treatment (ART) regimens; and (3) determine the risk factors for XDDIs with each regimen. A cross-sectional study was performed among adult HIV/HCV-coinfected patients. Demographics, comorbidities, and medication lists were collected from medical records. Medication lists were entered into Lexi-Interact drug interaction software and XDDI before/after the addition of SIM- and SOF-containing therapy was documented. Classification and regression tree (CART) analyses identified breakpoints in continuous variables. Before the addition of any HCV therapy, XDDIs were present in 20% of the 335 included patients. After the addition of SIM-containing therapy, the frequency of XDDIs significantly increased to 88.4% (p<0.001). After adding SOF-containing therapy, the prevalence of XDDIs increased to 24.5% (p<0.001). The prevalence of XDDIs was significantly lower for SOF-containing HCV therapy within various types of ART regimens. Use of ≥7 non-HIV medications (CART breakpoint) was the only variable to predict XDDIs before the addition of any HCV therapy. Similarly, this was the only variable to predict XDDIs after the addition of SOF-containing therapy (PR: 4.80; 95% CI: 2.57-8.96, p<0.001). Variables independently associated with XDDIs after the addition of SIM-containing therapy were NNRTI regimen (prevalence ratio, PR: 1.62; 95% confidence interval, CI: 1.38-1.91, p<0.001), PI regimen (PR: 1.64; 95% CI: 1.40-1.93, p<0.001), and ≥7 non-HIV medications (PR: 1.06; 95% CI: 1.00-1.14, p=0.09). The addition of SOF-containing therapy was associated with a lower prevalence of XDDI than SIM-containing therapy.
(1)理论上在患者用药清单中添加含西米普明(SIM)和索磷布韦(SOF)的治疗方案时,比较禁忌药物相互作用(XDDI)的发生频率;(2)确定在不同类型的抗逆转录病毒治疗(ART)方案中,哪种丙型肝炎(HCV)治疗方案与最低的XDDI发生频率相关;(3)确定每种治疗方案发生XDDI的危险因素。对成年HIV/HCV合并感染患者进行了一项横断面研究。从病历中收集人口统计学、合并症和用药清单。将用药清单录入Lexi-Interact药物相互作用软件,并记录添加含SIM和SOF治疗前后的XDDI情况。分类与回归树(CART)分析确定了连续变量的断点。在添加任何HCV治疗之前,335例纳入患者中有20%存在XDDI。添加含SIM治疗后,XDDI的发生频率显著增加至88.4%(p<0.001)。添加含SOF治疗后,XDDI的发生率增加至24.5%(p<0.001)。在各种ART方案中,含SOF的HCV治疗的XDDI发生率显著较低。在添加任何HCV治疗之前,使用≥7种非HIV药物(CART断点)是预测XDDI的唯一变量。同样,这也是添加含SOF治疗后预测XDDI的唯一变量(PR:4.80;95%CI:2.57-8.96,p<0.001)。添加含SIM治疗后,与XDDI独立相关的变量包括非核苷类逆转录酶抑制剂(NNRTI)方案(患病率比值,PR:1.62;95%置信区间,CI:1.38-1.91,p<0.001)、蛋白酶抑制剂(PI)方案(PR:1.64;95%CI:1.40-1.93,p<0.001)和≥7种非HIV药物(PR:1.06;95%CI:1.00-1.14,p=0.09)。与含SIM治疗相比,添加含SOF治疗与较低的XDDI患病率相关。
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