Department of Medicine, University of Washington, Seattle, Washington 98104, USA.
J Infect Dis. 2011 Aug 1;204(3):419-25. doi: 10.1093/infdis/jir264.
Mathematical models of hepatitis C virus (HCV) during therapy may elucidate mechanisms of action for antiviral therapy. In genome-wide association studies, IL28B gene polymorphisms are highly predictive of therapeutic clearance of HCV.
We collected sera from 20 chronically infected HCV participants at 13 points during the first 28 days of therapy. We assessed the presence of the C allele at single-nucleotide polymorphism rs12979860 using the ABI TaqMan allelic discrimination kit. We estimated dynamic parameters from the entire population using the Neumann model for HCV infection. Statistical methods for repeated nonlinear measures compared model parameters by established predictors of response.
The frequencies of IL28B genotypes were 6 (C/C), 11 (C/T), and 3 (T/T). The mean log decline in HCV RNA from 0 to 48 hours was more rapid among C/C genotype participants compared with C/T or T/T genotype participants (1.4 vs 0.7; P = .07), and from 2 days to 14 days (1.6 vs 0.7; P = .04). In the multivariate model, the C/C genotype predicted a steeper second-phase decline when adjusted for race (P = .01).
The presence of the C/C genotype at IL28B rs12979860 exerts its antiviral effect by increasing the infected hepatocyte death rate. This suggests that an immune-mediated mechanism is responsible.
丙型肝炎病毒(HCV)治疗期间的数学模型可以阐明抗病毒治疗的作用机制。在全基因组关联研究中,IL28B 基因多态性高度预测 HCV 治疗清除率。
我们在治疗的头 28 天内的 13 个时间点从 20 名慢性 HCV 感染者中采集血清。我们使用 ABI TaqMan 等位基因鉴别试剂盒评估单核苷酸多态性 rs12979860 处 C 等位基因的存在情况。我们使用 HCV 感染的 Neumann 模型从整个人群中估计动态参数。重复非线性测量的统计方法通过反应的既定预测因子比较模型参数。
IL28B 基因型的频率分别为 6(C/C)、11(C/T)和 3(T/T)。与 C/T 或 T/T 基因型参与者相比,C/C 基因型参与者从 0 到 48 小时 HCV RNA 的平均对数下降更快(1.4 与 0.7;P =.07),从 2 天到 14 天(1.6 与 0.7;P =.04)。在多变量模型中,当调整种族时,C/C 基因型预测第二阶段下降更陡峭(P =.01)。
IL28B rs12979860 处 C/C 基因型的存在通过增加感染肝细胞的死亡率发挥其抗病毒作用。这表明免疫介导的机制是负责的。
