病毒载量影响具有人源化免疫系统和肝脏的小鼠对乙肝病毒的免疫反应。
Viral Load Affects the Immune Response to HBV in Mice With Humanized Immune System and Liver.
作者信息
Dusséaux Mathilde, Masse-Ranson Guillemette, Darche Sylvie, Ahodantin James, Li Yan, Fiquet Oriane, Beaumont Elodie, Moreau Pierrick, Rivière Lise, Neuveut Christine, Soussan Patrick, Roingeard Philippe, Kremsdorf Dina, Di Santo James P, Strick-Marchand Helene
机构信息
Innate Immunity Unit, Institut Pasteur, 75724 Paris, France; INSERM U1223, Paris, France.
INSERM U1135, Faculté de Médecine, Université Pierre et Marie Curie Paris 6, Paris, France.
出版信息
Gastroenterology. 2017 Dec;153(6):1647-1661.e9. doi: 10.1053/j.gastro.2017.08.034. Epub 2017 Aug 26.
BACKGROUND & AIMS: Hepatitis B virus (HBV) infects hepatocytes, but the mechanisms of the immune response against the virus and how it affects disease progression are unclear.
METHODS
We performed studies with BALB/c Rag2Il2rgSirpaAlb-uPA mice, stably engrafted with human hepatocytes (HUHEP) with or without a human immune system (HIS). HUHEP and HIS-HUHEP mice were given an intraperitoneal injection of HBV. Mononuclear cells were isolated from spleen and liver for analysis by flow cytometry. Liver was analyzed by immunohistochemistry and mRNA levels were measured by quantitative reverse transcription polymerase chain reaction (PCR). Plasma levels of HBV DNA were quantified by PCR reaction, and antigen-specific antibodies were detected by immunocytochemistry of HBV-transfected BHK-21 cells.
RESULTS
Following HBV infection, a complete viral life cycle, with production of HBV DNA, hepatitis B e (HBe), core (HBc) and surface (HBs) antigens, and covalently closed circular DNA, was observed in HUHEP and HIS-HUHEP mice. HBV replicated unrestricted in HUHEP mice resulting in high viral titers without pathologic effects. In contrast, HBV-infected HIS-HUHEP mice developed chronic hepatitis with 10-fold lower titers and antigen-specific IgGs, (anti-HBs, anti-HBc), consistent with partial immune control. HBV-infected HIS-HUHEP livers contained infiltrating Kupffer cells, mature activated natural killer cells (CD69+), and PD-1+ effector memory T cells (CD45RO+). Reducing the viral inoculum resulted in more efficient immune control. Plasma from HBV-infected HIS-HUHEP mice had increased levels of inflammatory and immune-suppressive cytokines (C-X-C motif chemokine ligand 10 and interleukin 10), which correlated with populations of intrahepatic CD4+ T cells (CD45RO+PD-1+). Mice with high levels of viremia had HBV-infected liver progenitor cells. Giving the mice the nucleoside analogue entecavir reduced viral loads and decreased liver inflammation.
CONCLUSION
In HIS-HUHEP mice, HBV infection completes a full life cycle and recapitulates some of the immunopathology observed in patients with chronic infection. Inoculation with different viral loads led to different immune responses and levels of virus control. We found HBV to infect liver progenitor cells, which could be involved in hepatocellular carcinogenesis. This is an important new system to study anti-HBV immune responses and screen for combination therapies against hepatotropic viruses.
背景与目的
乙型肝炎病毒(HBV)感染肝细胞,但针对该病毒的免疫反应机制以及其如何影响疾病进展尚不清楚。
方法
我们对稳定植入有人肝细胞(HUHEP)且有或无人免疫系统(HIS)的BALB/c Rag2Il2rgSirpaAlb-uPA小鼠进行了研究。给HUHEP和HIS-HUHEP小鼠腹腔注射HBV。从脾脏和肝脏分离单核细胞,通过流式细胞术进行分析。通过免疫组织化学分析肝脏,并通过定量逆转录聚合酶链反应(PCR)测量mRNA水平。通过PCR反应定量血浆中HBV DNA水平,并通过对HBV转染的BHK-21细胞进行免疫细胞化学检测抗原特异性抗体。
结果
在HBV感染后,在HUHEP和HIS-HUHEP小鼠中观察到了完整的病毒生命周期,包括HBV DNA、乙型肝炎e抗原(HBe)、核心抗原(HBc)和表面抗原(HBs)的产生以及共价闭合环状DNA。HBV在HUHEP小鼠中不受限制地复制,导致高病毒滴度且无病理效应。相比之下,感染HBV的HIS-HUHEP小鼠发展为慢性肝炎,病毒滴度和抗原特异性IgG(抗-HBs、抗-HBc)降低10倍,这与部分免疫控制一致。感染HBV的HIS-HUHEP肝脏中含有浸润的库普弗细胞、成熟活化的自然杀伤细胞(CD69+)和PD-1+效应记忆T细胞(CD45RO+)。降低病毒接种量导致更有效的免疫控制。感染HBV的HIS-HUHEP小鼠血浆中炎症和免疫抑制细胞因子(C-X-C基序趋化因子配体10和白细胞介素10)水平升高,这与肝内CD4+ T细胞(CD45RO+PD-1+)群体相关。病毒血症水平高的小鼠有被HBV感染的肝祖细胞。给小鼠使用核苷类似物恩替卡韦可降低病毒载量并减轻肝脏炎症。
结论
在HIS-HUHEP小鼠中,HBV感染完成了完整的生命周期,并重现了慢性感染患者中观察到的一些免疫病理学特征。接种不同病毒载量导致不同的免疫反应和病毒控制水平。我们发现HBV可感染肝祖细胞,这可能与肝细胞癌发生有关。这是一个研究抗HBV免疫反应和筛选针对嗜肝病毒联合疗法的重要新系统。
Zotero 插件