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Modeling Ribavirin?¢????Induced Anemia in Patients with Chronic Hepatitis C Virus

机译:利巴韦林对慢性丙型肝炎病毒患者引起的贫血建模

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Ribavirin remains an important component of hepatitis C treatment in certain clinical scenarios, but it causes hemolytic anemia. A quantitative understanding of the ribavirin exposure?¢????anemia relationship is important in dose individualization/optimization. We developed a model relating ribavirin triphosphate (RTP) exposure in red blood cells (RBCs), RBC lifespan, feedback regulation of RBC production when anemia occurs, and the resulting hemoglobin decline. Inosine triphosphatase (ITPA) and interleukin 28B (IL28B) genetics were found to be significant covariates. Clinical trial simulations predicted that anemia is least severe in IL28B non?¢????CC (rs12979860, CT or TT), ITPA variant subjects, followed by IL28B non?¢????CC, ITPA wild?¢????type, IL28B CC, ITPA variant, and IL28B CC, ITPA wild?¢????type subjects (most severe). Reducing the ribavirin dose from 1,200/1,000 mg to 800/600 mg could reduce the proportions of grade 2 anemia by about half. The resulting model framework will aid the development of dosing strategies that minimize the incidence of anemia in treatment regimens that include ribavirin.
机译:利巴韦林在某些临床情况下仍是丙型肝炎治疗的重要组成部分,但会引起溶血性贫血。定量了解利巴韦林暴露与贫血的关系在剂量个体化/最优化中很重要。我们开发了一个模型,该模型与红细胞(RBC)中的利巴韦林三磷酸(RTP)暴露,RBC寿命,发生贫血时RBC产生的反馈调节以及导致的血红蛋白下降有关。发现肌苷三磷酸酶(ITPA)和白介素28B(IL28B)遗传学是重要的协变量。临床试验模拟预测,IL28B非CC(IT129变体),ITPA变异受试者的贫血最不严重,其次是IL28B非CC,ITPA野生型的贫血。 I型野生型,IL28B CC型和ITPA野生型IL28B CC型(最严重)。将利巴韦林的剂量从1,200 / 1,000 mg减少至800/600 mg,可以将2级贫血的比例降低约一半。由此产生的模型框架将有助于制定剂量策略,以最小化包括利巴韦林在内的治疗方案中贫血的发生率。

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