HIV co-infection and HCV-induced liver fibrosis in vivo

HIV合并感染和HCV诱导的体内肝纤维化

• 批准号: 8584278
• 负责人: Lishan Su
• 金额: $ 37万
• 依托单位: UNIV OF NORTH CAROLINA CHAPEL HILL
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-12-01 至 2016-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8584278
• 关键词: Acquired Immunodeficiency Syndrome; Address; Affect; Animal Model; B-Lymphocytes; Blood; CCR5 gene; Cell Culture Techniques; Cell physiology; Cells; Chronic; Coculture Techniques; Development; Engraftment; Fibrosis; Foundations; Future; Gene Expression; Genes; Genomics; Goals; HIV; HIV Infections; HIV-1; Hepatic; Hepatic Fibrogenesis; Hepatic Stellate Cell; Hepatitis; Hepatitis C; Hepatitis C virus; Hepatocyte; Human; Immune; Immune response; Immune system; Immunologics; In Vitro; Infection; Inflammation; Inflammatory Response; Kinetics; Knockout Mice; Light; Liver; Liver Cirrhosis; Liver Fibrosis; Liver diseases; Lymphoid; Measures; Mediating; Modeling; Monitor; Mus; Natural Killer Cells; Organ; Pan Genus; Pathogenesis; Patients; Play; Regulatory T-Lymphocyte; Reporting; Role; Stem cells; T cell response; T-Lymphocyte; Testing; Tissues; Transfection; Transgenes; Transplantation; Viral; Virus; Virus Replication; immune function; immunopathology; improved; in vivo; liver cell proliferation; liver inflammation; metabolomics; novel; novel therapeutics; prevent; stellate cell; suicidal; viral RNA

DESCRIPTION (provided by applicant): Hepatitis C virus (HCV) infection and HIV coinfection act synergistically to promote hepatic fibrosis and cirrhosis, but the underlying pathogenic mechanisms remain unclear due to a lack of appropriate animal models. The BalbC rag2/?C double knockout (DKO) mouse lacks T, B and NK cells and supports development of a functional human immune system in all lymphoid organs. To promote human liver cell co-engraftment, we introduced a liver-specific inducible suicidal transgene (AFC8) in the DKO mouse. Co-transplantation of human blood and liver progenitor cells in AFC8 mice leads to development of both human liver cells and immune cells in lymphoid/liver organs (AFC8-hu mice). These mice are permissive for HCV as well as HIV infection, support anti-viral human T cell responses, and develop human liver immunopathology (inflammation, hepatitis and fibrosis). I postulate that HIV co-infection may affect HCV-induced liver diseases by enhancing HCV replication; by elevating chronic hepatic inflammation; and by activating hepatic stellate cells to accelerate liver fibrosis. The AFC8-hu model is well suited for elucidating the mechanism underlying HCV/HIV synergy in human hepatic fibrosis in vivo. We propose the following aims: 1) The current AFC8-hu mouse will be improved to support higher human hepatocytes in the chimeric liver. In addition, HCV gt 1a and 2a clones will be tested to establish their infection and pathogenesis kinetics. 2) To study how HIV co-infection exacerbates HCV-induced liver fibrosis in AFC8-hu mice. We will define how HIV infection influences HCV infection, immunopathogenesis, stellate cell activation and liver fibrosis. In addition, the effectof HCV infection on HIV-1 replication and AIDS progression will also be monitored. 3) I propose that HIV coinfection dysregulates human inflammatory and immune responses to contribute to HCV-associated liver diseases. We will define the role of key HIV target cells pDC and Treg that promote HCV-induced liver stellate cell activation and fibrosis in vitro and in vivo. The novel AFC8-hu mouse is unique in providing a small animal model in which these important questions can be addressed. The answers to these questions will have a very significant impact on the field.

描述（由申请人提供）：丙型肝炎病毒（HCV）感染和HIV共感染与促进肝纤维化和肝硬化协同作用，但由于缺乏合适的动物模型，基本的致病机制尚不清楚。 BALBC RAG2/？C双基因敲除（DKO）小鼠缺乏T，B和NK细胞，并支持所有淋巴器官中功能性人体免疫系统的发展。为了促进人类肝细胞共晶，我们引入了DKO小鼠中的肝特异性自杀转基因（AFC8）。 AFC8小鼠中人体血液和肝脏祖细胞的共转移导致淋巴/肝脏器官（AFC8-HU小鼠）中人肝细胞和免疫细胞的发展。这些小鼠具有HCV和HIV感染，支持抗病毒人T细胞反应并发展人肝免疫病理学（炎症，肝炎和纤维化）。我假设HIV共感染可能会通过增强HCV复制来影响HCV诱导的肝脏疾病。通过升高慢性肝炎症；并通过激活肝星状细胞加速肝纤维化。 AFC8-HU模型非常适合阐明体内人肝纤维化中HCV/HIV协同的机制。我们提出以下目的：1）当前的AFC8-HU小鼠将得到改善，以支持嵌合肝脏中较高的人肝细胞。此外，将测试HCV GT 1A和2A克隆以建立 它们的感染和发病机理。 2）研究HIV共同感染如何加剧HCV诱导的AFC8-HU小鼠的肝纤维化。我们将定义HIV感染如何影响HCV感染，免疫致病发生，星状细胞活化和肝纤维化。另外，还将监测HCV感染对HIV-1复制和AIDS进展的影响。 3）我提出，HIV共感染失调的人类炎症和免疫反应会导致与HCV相关的肝脏疾病。我们将定义关键HIV靶细胞PDC和Treg的作用，从而促进HCV诱导的肝脏星状细胞活化和体外纤维化。新型的AFC8-HU鼠标在提供小型动物模型方面是独一无二的，可以解决这些重要问题。这些问题的答案将对该领域产生非常重大的影响。