Human Hepatocytes and Hematolymphoid Dual Reconstitution in Treosulfan-Conditioned uPA-NOG Mice

Gutti, Tanuja L.; Knibbe, Jaclyn; Makarov, Edward; Zhang, Jinjin; Yannam, Govardhana Rao; Gorantla, Santhi; Sun, Yimin; Mercer, David F.; Suemizu, Hiroshi; Wisecarver, James L.; Osna, Natalia A.; Bronich, Tatiana K.; Poluektova, Larisa Y.

doi:10.1016/j.ajpath.2013.09.008

Cited by 56 publications

(63 citation statements)

References 43 publications

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“…This has recently been reported by transplanting adult human hepatocytes and mismatched HSC derived from fetal human liver tissue, which resulted in doubly engrafted animals [7,8]. However, to avoid allogeneic immune responses both grafts should be derived from the same human donor.…”

Section: Introductionmentioning

confidence: 99%

“…Human HSC can also be obtained from adults [9] but hepatocytes from these same individuals are rarely available. When fetal hepatoblasts are combined with syngeneic HSC the liver graft either was lost [7] or the engrafted hepatoblasts fail to expand to high levels [10,11]. Together, these findings suggest that allogeneic doubly reconstituted mice can be generated but that human fetal hepatoblasts insufficiently engraft human liver chimeric mice, which limits the generation of syngeneic doubly reconstituted mice.…”

Section: Introductionmentioning

confidence: 99%

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Humanized mice efficiently engrafted with fetal hepatoblasts and syngeneic immune cells develop human monocytes and NK cells

Billerbeck

Mommersteeg

Shlomai

et al. 2016

Journal of Hepatology

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Background & Aims Human liver chimeric mice are useful models of human hepatitis virus infection, including hepatitis B and C virus infections. Independently, immunodeficient mice reconstituted with CD34+ hematopoietic stem cells (HSC) derived from fetal liver reliably develop human T and B lymphocytes. Combining these systems has long been hampered by inefficient liver reconstitution of human fetal hepatoblasts. Our study aimed to enhance hepatoblast engraftment in order to create a mouse model with syngeneic human liver and immune cells. Methods The effects of human oncostatin-M administration on fetal hepatoblast engraftment into immunodeficient fah−/− mice was tested. Mice were then transplanted with syngeneic human hepatoblasts and HSC after which human leukocyte chimerism and functionality were analyzed by flow cytometry, and mice were challenged with HBV. Results Addition of human oncostatin-M enhanced human hepatoblast engraftment in immunodeficient fah−/− mice by 5–100 fold. In contrast to mice singly engrafted with HSC, which predominantly developed human T and B lymphocytes, mice co-transplanted with syngeneic hepatoblasts also contained physiological levels of human monocytes and natural killer cells. Upon infection with HBV, these mice displayed rapid and sustained viremia. Conclusions Our study provides a new mouse model with improved human fetal hepatoblast engraftment and an expanded human immune cell repertoire. With further improvements, this model may become useful for studying human immunity against viral hepatitis. Lay summary Important human pathogens such as hepatitis B virus, hepatitis C virus and human immunodeficiency virus only infect human cells which complicates the development of mouse models for the study of these pathogens. One way to make mice permissive for human pathogens is the transplantation of human cells into immune-compromised mice. For instance, the transplantation of human liver cells will allow the infection of these so-called “liver chimeric mice” with hepatitis B virus and hepatitis C virus. The co-transplantation of human immune cells into liver chimeric mice will further allow the study of human immune responses to hepatitis B virus or hepatitis C virus. However, for immunological studies it will be crucial that the transplanted human liver and immune cells are derived from the same human donor. In our study we describe the efficient engraftment of human fetal liver cells and immune cells derived from the same donor into mice. We show that liver co-engraftment resulted in an expanded human immune cell repertoire, including monocytes and natural killer cells in the liver. We further demonstrate that these mice could be infected with hepatitis B virus, which lead to an expansion of natural killer cells. In conclusion we have developed a new mouse model that could be useful to study human immune responses to human liver pathogens.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Humanized mice efficiently engrafted with fetal hepatoblasts and syngeneic immune cells develop human monocytes and NK cells

Billerbeck

Mommersteeg

Shlomai

et al. 2016

Journal of Hepatology

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“…Engraftment efficiency appears to be strain-dependent as some studies report more robust engraftment with these fetal progenitor cells in AFC8 mice [25]. However, similar to liver transplantation in humans, close donor matching may not be imperative as it was recently shown that extensive humanization of both the liver and the immune system can been achieved through the use of allogeneic adult hepatocytes and HSCs without any overt rejection [34,35]. Dually engrafted mice mounted virus-specific immune responses following HBV infection, resulting in human-specific liver fibrosis [36].…”

Section: Host Adaptation: Xenotransplantation Modelsmentioning

confidence: 99%

Determinants of hepatitis B and delta virus host tropism

Winer

Ploß

2015

Current Opinion in Virology

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Hepatitis B virus (HBV) infections are a global health problem afflicting approximately 360 million patients. Of these individuals, 15–20 million are co-infected with hepatitis delta virus (HDV). Progress towards curative therapies has been impeded by the highly restricted host tropism of HBV, which is limited to productive infections in humans and chimpanzees. Here, we will discuss different approaches that have been taken to study HBV and HDV infections in vivo. The development of transgenic and humanized mice has lead to deeper insights into HBV pathogenesis. An improved understanding of the determinants governing HBV and HDV species tropism will aid the construction of a small animal model with inheritable susceptible to HBV/HDV.

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“…However, studies on HCV immunopathogenesis, primary (human) adaptive immune response and vaccine efficacy in mice would require both a human liver graft and a functional (human) immune system in one and the same recipient animal. This has recently been achieved by combining adult human hepatocytes and human CD34 + hematopoietic stem cells (HSCs) from different human donors [110,111]. Although the authors did not show HCV infection, the high human engraftment levels suggest that these mice could become viremic upon HCV challenge.…”

Section: Animal Models To Study Hcv Infectionmentioning

confidence: 99%

Animal models for the study of HCV

Vercauteren

Jong

Meuleman

2015

Current Opinion in Virology

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1 Summary The development and evaluation of effective therapies and vaccines for the hepatitis C virus (HCV) and the study of its interactions with the mammalian host have been hindered for a long time by the absence of suitable small animal models. Immune compromised mouse models that recapitulate the complete HCV life cycle have been useful to investigate many aspects of the HCV life cycle including antiviral interventions. However, HCV has a high propensity to establish persistence and associated histopathological manifestations such as steatosis, fibrosis, cirrhosis and hepatocellular carcinoma (HCC). Better understanding of these processes requires the development of a permissive and fully immunocompetent small animal model. In this review we summarize the in vivo models that are available for the study of HCV.

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Human Hepatocytes and Hematolymphoid Dual Reconstitution in Treosulfan-Conditioned uPA-NOG Mice

Cited by 56 publications

References 43 publications

Humanized mice efficiently engrafted with fetal hepatoblasts and syngeneic immune cells develop human monocytes and NK cells

Humanized mice efficiently engrafted with fetal hepatoblasts and syngeneic immune cells develop human monocytes and NK cells

Determinants of hepatitis B and delta virus host tropism

Animal models for the study of HCV

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