IL28B 基因型与慢性丙型肝炎患者肝内干扰素刺激基因的差异表达相关。
IL28B genotype is associated with differential expression of intrahepatic interferon-stimulated genes in patients with chronic hepatitis C.
机构信息
Center for Human Genome Variation, Duke University Medical Center, Durham, NC, USA.
出版信息
Hepatology. 2010 Dec;52(6):1888-96. doi: 10.1002/hep.23912. Epub 2010 Oct 7.
UNLABELLED
Genetic variation in the IL28B (interleukin 28B; interferon lambda 3) region has been associated with sustained virological response (SVR) rates in patients with chronic hepatitis C (CHC) who were treated with peginterferon-α and ribavirin. We hypothesized that IL28B polymorphism is associated with intrahepatic expression of interferon-stimulated genes (ISGs), known to influence treatment outcome. IL28B genotyping (rs12979860) and whole-genome RNA expression were performed using liver biopsies from 61 North American patients with CHC. After correction for multiple testing (false discovery rate < 0.10), 164 transcripts were found to be differentially expressed by IL28B-type. The interferon signaling pathway was the most enriched canonical pathway differentially expressed by IL28B-type (P < 10(-5)), with most genes showing higher expression in livers of individuals carrying the poor-response IL28B-type. In 25 patients for which treatment response data were available, IL28B-type was associated with SVR (P = 0.0054). ISG expression was also associated with SVR; however, this was not independent of IL28B-type. Analysis of miR-122 expression in liver biopsies showed reduced miR-122 levels associated with poorer treatment outcome, independently of IL28B-type. No association was observed between IL28B-type and levels of liver IL28B or IL28A messenger RNA expression. IL28B protein sequence variants associated with rs12979860 were therefore investigated in vitro: no differences in ISG induction or inhibition of HCV replication were observed in Huh7.5 cells.
CONCLUSION
The good response IL28B variant was strongly associated with lower level ISG expression. The results suggest that IL28B genotype may explain the relationship between hepatic ISG expression and HCV treatment outcome, and this is independent of miR-122 expression. IL28B-type was not associated with intrahepatic IL28B messenger RNA expression in vivo. Further investigation of the precise molecular mechanism(s) by which IL28B genetic variation influences HCV outcomes is warranted.
未加标注
白细胞介素 28B(IL28B;干扰素 lambda3)区域的遗传变异与接受聚乙二醇干扰素-α和利巴韦林治疗的慢性丙型肝炎(CHC)患者的持续病毒学应答(SVR)率有关。我们假设 IL28B 多态性与影响治疗结果的已知干扰素刺激基因(ISG)的肝内表达有关。使用来自 61 名北美 CHC 患者的肝活检进行了 IL28B 基因分型(rs12979860)和全基因组 RNA 表达分析。经过多次测试校正(错误发现率<0.10),发现 164 个转录本因 IL28B 型而差异表达。IL28B 型差异表达的最丰富的经典途径是干扰素信号通路(P<10(-5)),大多数基因在携带不良反应 IL28B 型的个体的肝脏中表达更高。在 25 名可获得治疗反应数据的患者中,IL28B 型与 SVR 相关(P=0.0054)。ISG 表达也与 SVR 相关;然而,这与 IL28B 型无关。对肝活检中 miR-122 表达的分析表明,miR-122 水平降低与较差的治疗结果相关,与 IL28B 型无关。未观察到 IL28B 型与肝 IL28B 或 IL28A 信使 RNA 表达水平之间存在关联。因此,在体外研究了与 rs12979860 相关的 IL28B 蛋白序列变异:在 Huh7.5 细胞中未观察到 ISG 诱导或抑制 HCV 复制的差异。
结论
良好反应的 IL28B 变异与较低水平的 ISG 表达强烈相关。结果表明,IL28B 基因型可能解释了肝内 ISG 表达与 HCV 治疗结果之间的关系,这与 miR-122 表达无关。在体内,IL28B 型与肝内 IL28B 信使 RNA 表达无关。进一步研究 IL28B 遗传变异影响 HCV 结局的确切分子机制是必要的。
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