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首页> 外文期刊>AIDS >The transforming growth factor-beta high-producer genotype is associated with response to hepatitis C virus-specific therapy in HIV-positive patients with acute hepatitis C.
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The transforming growth factor-beta high-producer genotype is associated with response to hepatitis C virus-specific therapy in HIV-positive patients with acute hepatitis C.

机译:HIV阳性急性丙型肝炎患者中,转化生长因子-β高产基因型与对丙型肝炎病毒特异性疗法的反应有关。

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BACKGROUND: Coinfection with the hepatitis C virus (HCV) in HIV-positive patients is an emerging health problem. The factors affecting response to HCV-specific therapy are poorly understood but may involve host genetic factors. HCV NS5A-induced inhibition of transforming growth factor-beta signaling has been suggested as a potential mechanism involved in HCV pathogenesis. Transforming growth factor-beta, a multifunctional cytokine, displays gene polymorphisms (transforming growth factor-beta codon 10T/C and codon 25G/C) associated with differential cytokine secretion. Here, we studied whether transforming growth factor-beta gene polymorphisms affect treatment response in HCV/HIV coinfection. METHODS: Transforming growth factor-beta genotypes were determined in 60 HIV-positive patients with acute hepatitis C treated with pegylated interferon-alpha. Patients were classified into those with a high-producer genotype and others with non-high-producer genotypes. Rates of sustained virological responses were compared between high-producer and non-high-producer patients. As a control, 100 healthy, 201 HIV(+)/HCV(-), and 148 HCV(+)/HIV(-) subjects were studied. RESULTS: Transforming growth factor-beta genotype distribution did not differ significantly between the groups. In HIV/HCV coinfection carriers of the transforming growth factor-beta high-producer genotype had significantly higher sustained virological response rates than patients with a transforming growth factor-beta non-high-producer genotype (75 vs. 41.7%; P = 0.039). In a forward-conditional stepwise regression model, transforming growth factor-beta high-producer genotype was confirmed as an independent positive predictor for sustained virological response in interferon-alpha therapy (odds ratio, 4.4; 95% confidence interval, 1.5-13.4; P = 0.009). CONCLUSION: Response rates to interferon-alpha therapy are enhanced in acute HCV-infected HIV-positive patients carrying the transforming growth factor-beta 'high-producer' genotype. This finding may indicate that a transforming growth factor-beta 'high-producer' state can partially compensate HCV NS5A-induced inhibition of transforming growth factor-beta signaling.
机译:背景:HIV阳性患者中的丙型肝炎病毒(HCV)合并感染是一个正在出现的健康问题。影响对HCV特异性疗法反应的因素了解甚少,但可能涉及宿主遗传因素。 HCV NS5A诱导的转化生长因子-β信号转导的抑制已被认为是参与HCV发病机理的潜在机制。转化生长因子-β,一种多功能的细胞因子,显示出与细胞因子分泌不同相关的基因多态性(转化生长因子-β密码子10T / C和25G / C密码子)。在这里,我们研究了转化生长因子-β基因多态性是否影响HCV / HIV合并感染的治疗反应。方法:确定了60例经聚乙二醇化干扰素-α治疗的急性丙型肝炎病毒感染阳性患者的转化生长因子-β基因型。将患者分为高生产者基因型患者和非高生产者基因型患者。比较高生产者和非高生产者患者的持续病毒学应答率。作为对照,研究了100名健康的201名HIV(+)/ HCV(-)和148名HCV(+)/ HIV(-)受试者。结果:两组间转化生长因子-β基因型分布无明显差异。在HIV / HCV合并感染中,转化生长因子-β高产基因型的携带者的持续病毒学应答率显着高于转化生长因子-β非高产基因型的患者(75比41.7%; P = 0.039) 。在前向条件逐步回归模型中,转化生长因子-β高生产者基因型被确认为干扰素-α治疗中持续病毒学应答的独立阳性预测因子(赔率,4.4; 95%置信区间,1.5-13.4; P = 0.009)。结论:携带转化生长因子-β“高生产者”基因型的急性HCV感染的HIV阳性患者,对干扰素-α疗法的反应率提高。这一发现可能表明,转化生长因子-β“高产”状态可以部分补偿HCV NS5A诱导的转化生长因子-β信号转导的抑制。

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