首页> 美国卫生研究院文献>Journal of Virology >Deficiencies in the Acute-Phase Cell-Mediated Immune Response to Viral Antigens Are Associated with Development of Chronic Woodchuck Hepatitis Virus Infection following Neonatal Inoculation
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Deficiencies in the Acute-Phase Cell-Mediated Immune Response to Viral Antigens Are Associated with Development of Chronic Woodchuck Hepatitis Virus Infection following Neonatal Inoculation

机译:新生儿接种疫苗后急性病毒介导的急性期细胞介导的免疫反应的缺陷与慢性土拨鼠肝炎病毒感染的发展有关。

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摘要

In vitro proliferation of peripheral blood mononuclear cells was used to measure virus-specific cell-mediated immunity (vCMI) following neonatal woodchuck hepatitis virus (WHV) infection. Fifteen neonates were inoculated with the W8 strain of WHV. In 11, infection was resolved, and 4 became chronic carriers. Nineteen neonates were inoculated with the W7 strain and all became chronic carriers. Seven age-matched uninfected woodchucks served as controls. Virologic and vCMI profiles among the W8 and W7 infections were compared and related to the outcome of infection. Resolving woodchucks had robust, acute-phase vCMI to WHV antigens (core, surface, and x) and to several nonoverlapping core peptides. The acute-phase vCMI was associated temporally with the clearance of viral DNA and of surface antigen from serum at 14 to 22 weeks postinfection. In contrast, in approximately half of the W8 and W7 infections that progressed to chronicity, no significant acute-phase vCMI was detected. In the remaining carriers, acute-phase vCMI was observed, but it was less frequent and incomplete compared to that of resolved woodchucks. Serum viral load developed less rapidly in those carriers that had evidence of acute-phase vCMI, but it was still increased compared to that of resolving woodchucks. Thus, vigorous and multispecific acute-phase vCMI was associated with resolution of neonatal WHV infection. Absent or incomplete acute-phase vCMI was associated with the progression to chronic infection. By analogy, these results suggest that the onset of chronic hepatitis B virus (HBV) infection in humans may be associated with deficiencies in the primary T-cell response to acute HBV infection.
机译:新生儿土拨鼠肝炎病毒(WHV)感染后,外周血单核细胞的体外增殖用于测量病毒特异性细胞介导的免疫(vCMI)。用WHV的W8株接种15例新生儿。在11个地区,感染得到解决,有4个成为慢性携带者。 W19株接种了19例新生儿,并且全部成为慢性携带者。七个年龄匹配的未感染的土拨鼠作为对照。比较了W8和W7感染中的病毒学和vCMI配置文件,并将其与感染的结果相关。解决的土拨鼠对WHV抗原(核心,表面和x)以及几种不重叠的核心肽具有牢固的急性期vCMI。在感染后14至22周,急性期vCMI暂时与血清中病毒DNA和表面抗原的清除相关。相反,在进展为慢性的W8和W7感染中,大约有一半未检测到明显的急性期vCMI。在其余的携带者中,观察到急性期的vCMI,但与已解决的土拨鼠相比,它的发生频率较低且不完整。在有急性期vCMI证据的携带者中,血清病毒载量的发展较慢,但与解决土拨鼠相比,病毒载量仍增加了。因此,有力的多特异性急性期vCMI与新生儿WHV感染的消退有关。急性期vCMI的缺乏或不完全与慢性感染的进展有关。以此类推,这些结果表明,人类慢性乙型肝炎病毒(HBV)感染的发作可能与对急性HBV感染的原代T细胞反应缺乏有关。

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