急性丙型肝炎病毒感染会导致循环微RNA发生一致变化,这些变化与非溶解性肝细胞释放有关。
Acute Hepatitis C Virus Infection Induces Consistent Changes in Circulating MicroRNAs That Are Associated with Nonlytic Hepatocyte Release.
作者信息
El-Diwany Ramy, Wasilewski Lisa N, Witwer Kenneth W, Bailey Justin R, Page Kimberly, Ray Stuart C, Cox Andrea L, Thomas David L, Balagopal Ashwin
机构信息
Department of Medicine Division of Infectious Diseases, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
Department of Molecular and Comparative Pathobiology, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
出版信息
J Virol. 2015 Sep;89(18):9454-64. doi: 10.1128/JVI.00955-15. Epub 2015 Jul 8.
UNLABELLED
Plasma microRNAs (miRNAs) change in abundance in response to disease and have been associated with liver fibrosis severity in chronic hepatitis C virus (HCV) infection. However, the early dynamics of miRNA release during acute HCV infection are poorly understood. In addition, circulating miRNA signatures have been difficult to reproduce among separate populations. We studied plasma miRNA abundance during acute HCV infection to identify an miRNA signature of early infection. We measured 754 plasma miRNAs by quantitative PCR array in a discovery cohort of 22 individuals before and during acute HCV infection and after spontaneous resolution (n = 11) or persistence (n = 11) to identify a plasma miRNA signature. The discovery cohort derived from the Baltimore Before and After Acute Study of Hepatitis. During acute HCV infection, increases in miR-122 (P < 0.01) and miR-885-5p (Pcorrected < 0.05) and a decrease in miR-494 (Pcorrected < 0.05) were observed at the earliest time points after virus detection. Changes in miR-122 and miR-885-5p were sustained in persistent (P < 0.001) but not resolved HCV infection. The circulating miRNA signature of acute HCV infection was confirmed in a separate validation cohort that was derived from the San Francisco-based You Find Out (UFO) Study (n = 28). As further confirmation, cellular changes of signature miRNAs were examined in a tissue culture model of HCV in hepatoma cells: HCV infection induced extracellular release of miR-122 and miR-885-5p despite unperturbed intracellular levels. In contrast, miR-494 accumulated intracellularly (P < 0.05). Collectively, these data are inconsistent with necrolytic release of hepatocyte miRNAs into the plasma during acute HCV infection of humans.
IMPORTANCE
MicroRNAs are small noncoding RNA molecules that emerging research shows can transmit regulatory signals between cells in health and disease. HCV infects 2% of humans worldwide, and chronic HCV infection is a major cause of severe liver disease. We profiled plasma miRNAs in injection drug users before, during, and (in the people with resolution) after HCV infection. We discovered miRNA signatures of acute and persistent viremia and confirmed these findings two ways: (i) in a separate cohort of people with newly acquired HCV infection and (ii) in an HCV cell culture system. Our results demonstrate that acute HCV infection induces early changes in the abundance of specific plasma miRNAs that may affect the host response to HCV infection.
未标注
血浆微小RNA(miRNA)的丰度会因疾病而改变,并且已被证明与慢性丙型肝炎病毒(HCV)感染中的肝纤维化严重程度相关。然而,急性HCV感染期间miRNA释放的早期动态变化却鲜为人知。此外,循环miRNA特征在不同人群中难以重现。我们研究了急性HCV感染期间血浆miRNA的丰度,以确定早期感染的miRNA特征。我们通过定量PCR阵列在22名个体的发现队列中测量了754种血浆miRNA,这些个体在急性HCV感染之前、期间以及自发缓解(n = 11)或持续感染(n = 11)之后进行检测,以确定血浆miRNA特征。该发现队列来自巴尔的摩急性肝炎前后研究。在急性HCV感染期间,在病毒检测后的最早时间点观察到miR-122(P < 0.01)和miR-885-5p(校正后P < 0.05)增加,而miR-494(校正后P < 0.05)减少。miR-122和miR-885-5p的变化在持续感染(P < 0.001)中持续存在,但在已缓解的HCV感染中未持续。急性HCV感染的循环miRNA特征在另一个来自旧金山“你发现了(UFO)研究”的验证队列(n = 28)中得到证实。作为进一步的确认,在肝癌细胞的HCV组织培养模型中检查了特征性miRNA的细胞变化:尽管细胞内水平未受干扰,但HCV感染诱导了miR-122和miR-885-5p的细胞外释放。相比之下,miR-494在细胞内积累(P < 0.05)。总体而言,这些数据与人类急性HCV感染期间肝细胞miRNA向血浆中的坏死性释放不一致。
重要性
微小RNA是小的非编码RNA分子,新兴研究表明它们可以在健康和疾病状态下在细胞之间传递调节信号。HCV感染全球2%的人口,慢性HCV感染是严重肝脏疾病的主要原因。我们在注射吸毒者中对HCV感染之前、期间以及(在缓解者中)之后的血浆miRNA进行了分析。我们发现了急性和持续性病毒血症的miRNA特征,并通过两种方式证实了这些发现:(i)在另一个新感染HCV的人群队列中,以及(ii)在HCV细胞培养系统中。我们的结果表明,急性HCV感染会诱导特定血浆miRNA丰度的早期变化,这可能会影响宿主对HCV感染的反应。
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