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Tolerability of Erythrocyte Ribavirin Triphosphate Concentrations Depends on the ITPA Genotype

机译:红细胞利巴韦林三磷酸浓度的可耐受性取决于ITPA基因型

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Background: Ribavirin (RBV) is an antiviral drug that is part of the current standard therapy for chronic hepatitis C (CHC). It is enzymat-ically converted to ribavirin triphosphate (RTP) that inhibits the activity of viral RNA polymerase, thereby preventing viral replication. However, one of its adverse effects includes hemolytic anemia that limits its application. The variant of ITPA (inosine triphosphatase), which dephos-phorylates inosine triphosphate to inosine monophosphate, is a protective factor for RBV-induced anemia. RTP is an important metabolite required for ribavirin action. This study evaluated the time-dependent association of RTP concentrations in erythrocytes, RBV-induced toxic-ity, and virological response to RBV treatment for hepatitis C. Methods: A total of 28 Japanese patients with CHC were treated with RBV/peg-interferon/simeprevir or RBV/sofosbuvir and were genotyped for ITPA variants (rs1127354 and rs7270101). We measured RTP concentrations in erythrocytes in a total of 76 samples collected at 4, 8, and 12 weeks from the initiation of treatment. Results: The ITPA rs1 127354 variant was found in 7 patients. This was associated with significantly higher RTP concentrations in erythrocytes than in the wild-type patients (P , 0.001). Moreover, a significant correlation was observed between RTP concentrations and decline in hemoglobin (Hb) levels from baseline values in ITPA wild type and rs1 127354 variant 12 weeks after treatment initiation (P , 0.01; r = 20.618 and 20.967, respectively). Multiple regression analysis revealed that ITPA genotype and erythrocyte RTP concentrations were major factors associated with reduced Hb levels in RBV therapy for CHC. However, we did not find any association between erythrocyte concentrations and virological response. Conclusions: The increased tolerability to RTP concentrations in erythrocytes in the ITPA variant rs1 127354 plays a role in preventing RBV-induced severe anemia in this ITPA variant.
机译:背景:利巴韦林(RBV)是一种抗病毒药物,是慢性丙型肝炎(CHC)目前标准治疗的一部分。酶促转化为抑制病毒RNA聚合酶活性的利巴韦林三磷酸(RTP),从而防止病毒复制。然而,其一种不良反应之一包括限制其应用的溶血性贫血。 Dephos-phorlylates inosine三磷酸肌苷对Inosine单磷酸盐的变体,是RBV诱导的贫血血症的保护因子。 RTP是利巴林素作用所需的重要代谢物。该研究评估了RTP浓度在红细胞,RBV诱导的毒性型和病毒学反应对丙型肝炎的毒性治疗中的时间依赖性关联。方法:使用RBV / PEG - 干扰素(RBV / PEG-Welleron)治疗共28例CHC患者/ SIMEPREVIR或RBV / SOFOSBUVIR并进行ITPA变体的基因分型(RS1127354和RS7270101)。我们在4,8和12周内测量红细胞中的RTP浓度,从开始处理的4,8和12周中收集的76个样品。结果:7例患者发现ITPA RS1 127354变体。这与红细胞中的显着高于野生型患者(P,0.001)中明显较高的RTP浓度有关。此外,在治疗开始后12周的ITPA野生型和RS1 127354变体的基线值与基线值的血红蛋白(HB)水平之间观察到显着相关性并分别分别从AITPA野生型和RS1 127354变体中的血红蛋白(HB)水平。多元回归分析显示ITPA基因型和红细胞RTP浓度是与CHC的RBV治疗中的HB水平降低的主要因素。但是,我们没有发现红细胞浓度与病毒学反应之间的任何关联。结论:ITPA变体RS1 127354中红细胞中RTP浓度的增加的可耐受性在预防该ITPA变体中的RBV诱导的严重贫血中起着作用。

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