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首页> 外文期刊>The Journal of Clinical Investigation: The Official Journal of the American Society for Clinical Investigation >IL-21 is pivotal in determining age-dependent effectiveness of immune responses in a mouse model of human hepatitis B.
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IL-21 is pivotal in determining age-dependent effectiveness of immune responses in a mouse model of human hepatitis B.

机译:IL-21 在确定人类乙型肝炎小鼠模型中免疫反应的年龄依赖性有效性方面至关重要。

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摘要

HBV is a noncytopathic hepadnavirus and major human pathogen that causes immune-mediated acute and chronic hepatitis. The immune response to HBV antigens is age dependent: viral clearance occurs in most adults, while neonates and children usually develop chronic infection and liver disease. Here, we characterize an animal model for HBV infection that recapitulates the key differences in viral clearance between early life and adulthood and find that IL-21 may be part of an effective primary hepatic immune response to HBV. In our model, adult mice showed higher HBV-dependent IL-21 production in liver, compared with that of young mice. Conversely, absence of the IL-21 receptor in adult mice resulted in antigen persistence akin to that of young mice. In humans, levels of IL-21 transcripts were greatly increased in blood samples from acutely infected adults who clear the virus. These observations suggest a different model for the dichotomous, age dependent outcome of HBV infection in humans, in which decreased IL-21 production in younger patients may hinder generation of crucial CD8+ T and B cell responses. These findings carry implications for therapeutic augmentation of immune responses to HBV and potentially other persistent liver viruses.
机译:乙型肝炎病毒是一种非细胞病性肝病毒,也是引起免疫介导的急性和慢性肝炎的主要人类病原体。对HBV抗原的免疫反应与年龄有关:大多数成人都会清除病毒,而新生儿和儿童通常会发展为慢性感染和肝病。在这里,我们表征了HBV感染的动物模型,该模型概括了生命早期和成年期之间病毒清除的主要差异,并发现IL-21可能是对HBV的有效原发性肝脏免疫反应的一部分。在我们的模型中,与年轻小鼠相比,成年小鼠在肝脏中表现出更高的HBV依赖性IL-21产生。相反,成年小鼠中IL-21受体的缺失导致抗原持久性类似于年轻小鼠。在人类中,清除病毒的急性感染成人的血液样本中IL-21转录物的水平大大增加。这些观察结果表明,人类 HBV 感染的二分类、年龄依赖性结果存在一种不同的模型,其中年轻患者 IL-21 产生的减少可能会阻碍关键 CD8+ T 和 B 细胞反应的产生。这些发现对治疗性增强对HBV和潜在的其他持久性肝病毒的免疫反应具有重要意义。

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