Interferon Alpha-Inducible Protein 27 Expression Is Linked to Disease Severity in Chronic Infection of Both HIV-1 and HIV-2

IF 2 Q4 VIROLOGY
A. Palm, Srinivas Veerla, Jacob Lindman, P. Isberg, Emil Johansson, Antonio J. Biague, F. Månsson, H. Norrgren, J. Esbjörnsson, P. Medstrand, M. Jansson
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引用次数: 4

Abstract

Disease progression is slower in HIV-2, as compared with HIV-1 infection, in accordance with low or undetectable plasma viremia at viral setpoint. However, it is unclear why most HIV-2 infected individuals are still at risk of developing AIDS. To explore if specific host responses are linked to HIV disease severity, we have compared blood gene expression profiles between HIV seronegative and HIV-1, HIV-2 or dually HIV-1/HIV-2 infected individuals. In this study the gene encoding Interferon alpha-inducible protein 27 (IFI27) was found to be the most differentially expressed. Detailed expression analysis revealed significantly higher IFI27 expression in HIV infected individuals compared with seronegative individuals, irrespectively of HIV type. Moreover, IFI27 expression was higher in HIV-1 than in HIV-2 infected individuals. Multiple linear regression analysis, adjusting for age and sex, showed also that plasma viral load was the strongest predictor of IFI27 expression, followed by CD4% and HIV type. In line with this, IFI27 expression was found to be higher in HIV-2 viremic, compared with HIV-2 aviremic individuals. Still, HIV-2 aviremic individuals displayed elevated IFI27 expression compared with seronegative individuals. Furthermore, in HIV-2 infected individuals, IFI27 expression was also correlated with plasma markers previously linked to inflammation and disease progression in HIV infection. Taken together, our findings suggest that sustained elevation of type I interferon signaling, here reflected by elevated IFI27 expression in the chronic infection phase, is a key pathogenic feature of both HIV-1 and HIV-2.
干扰素α诱导蛋白27的表达与HIV-1和HIV-2慢性感染的疾病严重程度有关
与HIV-1感染相比,HIV-2感染的疾病进展较慢,这与病毒设定值低或检测不到的血浆病毒血症有关。然而,目前尚不清楚为什么大多数HIV-2感染者仍然有发展为艾滋病的风险。为了探索特异性宿主反应是否与HIV疾病严重程度有关,我们比较了HIV血清阴性和HIV-1、HIV-2或双重HIV-1/HIV-2感染者之间的血液基因表达谱。在本研究中发现编码干扰素α诱导蛋白27 (IFI27)的基因是差异表达最多的。详细的表达分析显示,与HIV类型无关,HIV感染者中if27的表达明显高于血清阴性个体。此外,IFI27在HIV-1感染个体中的表达高于HIV-2感染个体。对年龄和性别进行调整后的多元线性回归分析也显示,血浆病毒载量是IFI27表达的最强预测因子,其次是CD4%和HIV类型。与此相一致的是,与HIV-2病毒血症个体相比,IFI27在HIV-2病毒血症中的表达更高。尽管如此,与血清阴性个体相比,HIV-2病毒血症个体表现出升高的if27表达。此外,在HIV-2感染个体中,IFI27的表达也与先前与HIV感染炎症和疾病进展相关的血浆标志物相关。综上所述,我们的研究结果表明,I型干扰素信号的持续升高,在慢性感染阶段通过IFI27表达的升高来反映,是HIV-1和HIV-2的一个关键致病特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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