Your search keyword '"LIVER CHIMERIC MICE"' showing total 9 results

1. Liver chimeric mice with tupaia hepatocyte transplantation as an animal model for hepatitis B virus infection and antiviral therapy

Author

Lunzhi Yuan, Yao Chen, Xuan Liu, Yali Zhang, Ming Zhou, Kun Wu, Quan Yuan, Tong Cheng, and Ningshao Xia

Subjects

Tupaia, Hepatitis B, Liver chimeric mice, Infectious animal model, Antiviral therapy, Infectious and parasitic diseases, RC109-216, Public aspects of medicine, RA1-1270

Abstract

The human liver chimeric mouse is a milestone animal model for hepatitis B virus (HBV) infection. Such mice with primary human hepatocyte (PHH) transplantation are adequate to support chronic HBV infection for several weeks and to evaluate antiviral drugs. However, the drawbacks of PHHs include lack of available donors, poor expansion in vitro and ethical issues that limit the application of human liver chimeric mice, necessitating the search for alternatives. Here, we transplanted primary tupaia hepatocytes (PTHs) into the livers of immunodeficient mice and achieved high liver chimerism within six weeks. These tupaia liver chimeric mice are adequate to support chronic infection of the four common HBV genotypes A, B, C and D for 36 weeks, as well as evaluate of antiviral drugs, including hepatitis B immune globulin (HBIG), monoclonal antibody and nucleoside analogues (NAs), for preventative therapy and treatment post infection. In conclusion, the tupaia liver chimeric mouse model provides a convenient, efficient and stable animal model for chronic HBV infection and long-term drug evaluation.

Published

2019

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

Author

Billerbeck, Eva, Mommersteeg, Michiel C., Shlomai, Amir, Xiao, Jing W., Andrus, Linda, Bhatta, Ankit, Vercauteren, Koen, Michailidis, Eleftherios, Dorner, Marcus, Krishnan, Anuradha, Charlton, Michael R., Chiriboga, Luis, Rice, Charles M., and de Jong, Ype P.

Subjects

*LABORATORY mice, *MONOCYTES, *KILLER cells, *LYMPHOCYTES, *CHIMERISM

Abstract

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. [ABSTRACT FROM AUTHOR]

Published

2016

3. Liver chimeric mice with tupaia hepatocyte transplantation as an animal model for hepatitis B virus infection and antiviral therapy

Author

Kun Wu, Ningshao Xia, Yali Zhang, Tong Cheng, Ming Zhou, Xuan Liu, Quan Yuan, Lunzhi Yuan, and Yao Chen

Subjects

Microbiology (medical), Drug, medicine.drug_class, media_common.quotation_subject, Tupaia, Antiviral therapy, medicine.disease_cause, Monoclonal antibody, lcsh:Infectious and parasitic diseases, Medicine, lcsh:RC109-216, media_common, Hepatitis B virus, Hepatitis B immune globulin, biology, business.industry, lcsh:Public aspects of medicine, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, biology.organism_classification, Hepatitis B, Virology, In vitro, Transplantation, Chronic infection, Infectious Diseases, Infectious animal model, business, Liver chimeric mice, Biotechnology, medicine.drug

Abstract

The human liver chimeric mouse is a milestone animal model for hepatitis B virus (HBV) infection. Such mice with primary human hepatocyte (PHH) transplantation are adequate to support chronic HBV infection for several weeks and to evaluate antiviral drugs. However, the drawbacks of PHHs include lack of available donors, poor expansion in vitro and ethical issues that limit the application of human liver chimeric mice, necessitating the search for alternatives. Here, we transplanted primary tupaia hepatocytes (PTHs) into the livers of immunodeficient mice and achieved high liver chimerism within six weeks. These tupaia liver chimeric mice are adequate to support chronic infection of the four common HBV genotypes A, B, C and D for 36 weeks, as well as evaluate of antiviral drugs, including hepatitis B immune globulin (HBIG), monoclonal antibody and nucleoside analogues (NAs), for preventative therapy and treatment post infection. In conclusion, the tupaia liver chimeric mouse model provides a convenient, efficient and stable animal model for chronic HBV infection and long-term drug evaluation.

Published

2019

4. Innovations, challenges, and minimal information for standardization of humanized mice

Subjects

HEPATITIS-B, regenerative medicine, BREAST-CANCER CELLS, MOUSE MODEL, VIRUS-INFECTION, humanized mice, HUMAN HEPATOCYTES, XENOGRAFTS, HEMATOPOIETIC STEM-CELLS, IMMUNE-SYSTEM, infections, immuno-oncology, LIVER CHIMERIC MICE, PDX, ANTIBODY THERAPY

Abstract

Mice xenotransplanted with human cells and/or expressing human gene products (also known as "humanized mice") recapitulate the human evolutionary specialization and diversity of genotypic and phenotypic traits. These models can provide a relevantin vivocontext for understanding of human-specific physiology and pathologies. Humanized mice have advanced toward mainstream preclinical models and are now at the forefront of biomedical research. Here, we considered innovations and challenges regarding the reconstitution of human immunity and human tissues, modeling of human infections and cancer, and the use of humanized mice for testing drugs or regenerative therapy products. As the number of publications exploring different facets of humanized mouse models has steadily increased in past years, it is becoming evident that standardized reporting is needed in the field. Therefore, an international community-driven resource called "Minimal Information for Standardization of Humanized Mice" (MISHUM) has been created for the purpose of enhancing rigor and reproducibility of studies in the field. WithinMISHUM, we propose comprehensive guidelines for reporting critical information generated using humanized mice.

Published

2020

5. Innovations, challenges, and minimal information for standardization of humanized mice

Author

Michael A. Brehm, Carol J. Bult, Johannes Sam, Florian Klein, Silvia Guionaud, Karl-Dimiter Bissig, James P. Di Santo, Anja Kathrin Wege, Terrence Meeham, Dominique Bonnet, Scott G. Kitchen, Livio Trusolino, Kourosh Saeb-Parsy, Christian Münz, Brian Soper, Kristina E. Howard, Amar Deep Sharma, Renata Stripecke, Estefanía Rodríguez, Leonard D. Shultz, Li-Chin Yao, Andreas Trumpp, Jan Jacob Schuringa, University of Zurich, Stripecke, Renata, Stripecke, Renata [0000-0001-7756-8460], Münz, Christian [0000-0001-6419-1940], Schuringa, Jan Jacob [0000-0001-8452-8555], Trumpp, Andreas [0000-0002-6212-3466], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Medicine (General), Standardization, HEPATITIS-B, Review, Mice, SCID, QH426-470, 10263 Institute of Experimental Immunology, Regenerative medicine, Chromatin, Epigenetics, Genomics & Functional Genomics, immuno‐oncology, Mice, 0302 clinical medicine, Neoplasms, Medicine, infections, LIVER CHIMERIC MICE, BREAST-CANCER CELLS, MOUSE MODEL, humanized mice, Molecular Medicine, Heterografts, Immunology, regenerative medicine, Context (language use), 610 Medicine & health, Guidelines as Topic, VIRUS-INFECTION, Computational biology, 03 medical and health sciences, R5-920, Genetics, XENOGRAFTS, immuno-oncology, PDX, Animals, Humans, HEMATOPOIETIC STEM-CELLS, business.industry, Reproducibility of Results, Disease Models, Animal, HUMAN HEPATOCYTES, 030104 developmental biology, 1313 Molecular Medicine, Humanized mouse, 570 Life sciences, biology, IMMUNE-SYSTEM, Breast cancer cells, Antibody therapy, business, 030217 neurology & neurosurgery, ANTIBODY THERAPY

Abstract

Mice xenotransplanted with human cells and/or expressing human gene products (also known as “humanized mice”) recapitulate the human evolutionary specialization and diversity of genotypic and phenotypic traits. These models can provide a relevant in vivo context for understanding of human‐specific physiology and pathologies. Humanized mice have advanced toward mainstream preclinical models and are now at the forefront of biomedical research. Here, we considered innovations and challenges regarding the reconstitution of human immunity and human tissues, modeling of human infections and cancer, and the use of humanized mice for testing drugs or regenerative therapy products. As the number of publications exploring different facets of humanized mouse models has steadily increased in past years, it is becoming evident that standardized reporting is needed in the field. Therefore, an international community‐driven resource called “Minimal Information for Standardization of Humanized Mice” (MISHUM) has been created for the purpose of enhancing rigor and reproducibility of studies in the field. Within MISHUM, we propose comprehensive guidelines for reporting critical information generated using humanized mice., Humanized mice are at the forefront of biomedical research and becoming more mainstream preclinical models. This comprehensive review talks about innovations and challenges regarding the reconstitution of human immunity and introduces “Minimal Information for Standardization of Humanized Mice” (MISHUM).

Published

2020

6. Robust hepatitis E virus infection and transcriptional response in human hepatocytes

Author

Vanessa M. Pfankuche, Joerg Steinmann, Leonard Knegendorf, Patrick Behrendt, Nora Moeller, Yannick Brüggemann, Philip Meuleman, Wolfgang Baumgärtner, Daniel Todt, Thomas L Burkard, Florian W. R. Vondran, Michael Engelmann, Lieven Verhoye, Volker Kinast, Rani Burm, Martina Friesland, Avista Wahid, Eike Steinmann, Dimas F. Praditya, Toni Luise Meister, Christina Puff, and TWINCORE, Zentrum für experimentelle und klinische Infektionsforschung GmbH,Feodor-Lynen Str. 7, 30625 Hannover, Germany.

Subjects

Swine, viruses, PATHOGENESIS, Cell Culture Techniques, Medizin, Orthohepevirus, medicine.disease_cause, Virus Replication, chemistry.chemical_compound, Mice, transcriptomics, 0302 clinical medicine, Hepatitis E virus, Medicine and Health Sciences, LIVER CHIMERIC MICE, 0303 health sciences, Multidisciplinary, biology, Liver Neoplasms, virus diseases, Hep G2 Cells, Viral Load, Biological Sciences, Hepatitis E, 3. Good health, humanized mice, 030211 gastroenterology & hepatology, Viral hepatitis, Carcinoma, Hepatocellular, Genotype, NEW-MODELS, Antiviral Agents, Microbiology, Virus, 03 medical and health sciences, Viral life cycle, Cell Line, Tumor, Ribavirin, medicine, Animals, Humans, primary hepatocytes, 030304 developmental biology, Biology and Life Sciences, biology.organism_classification, medicine.disease, RNA-Dependent RNA Polymerase, Virology, digestive system diseases, infection, LIFE-CYCLE, Hepeviridae, chemistry, REPLICATION, Hepatocytes, hepatitis E virus (HEV), Replicon

Abstract

Significance Chronic HEV infections pose a significant clinical problem in immunocompromised individuals. The lack of an efficient cell culture system has severely limited investigation of the HEV life cycle and the development of effective antivirals. Here we report the establishment of a robust HEV cell culture system in human hepatocytes with viral titers up to 106 FFU/mL. These produced intracellular-derived HEVcc particles demonstrated replication to high viral loads in human liver chimeric mice and were able to efficiently infect primary human as well as porcine hepatocytes. This unique infectious cell culture model provides a powerful tool for the analysis of host–virus interactions that should facilitate the discovery of antiviral drugs for this important zoonotic pathogen., Hepatitis E virus (HEV) is the causative agent of hepatitis E in humans and the leading cause for acute viral hepatitis worldwide. The virus is classified as a member of the genus Orthohepevirus A within the Hepeviridae family. Due to the absence of a robust cell culture model for HEV infection, the analysis of the viral life cycle, the development of effective antivirals and a vaccine is severely limited. In this study, we established a protocol based on the HEV genotype 3 p6 (Kernow C-1) and the human hepatoma cell lines HepG2 and HepG2/C3A with different media conditions to produce intracellular HEV cell culture-derived particles (HEVcc) with viral titers between 105 and 106 FFU/mL. Viral titers could be further enhanced by an HEV variant harboring a mutation in the RNA-dependent RNA polymerase. These HEVcc particles were characterized in density gradients and allowed the trans-complementation of subgenomic reporter HEV replicons. In addition, in vitro produced intracellular-derived particles were infectious in liver-humanized mice with high RNA copy numbers detectable in serum and feces. Efficient infection of primary human and swine hepatocytes using the developed protocol could be observed and was inhibited by ribavirin. Finally, RNA sequencing studies of HEV-infected primary human hepatocytes demonstrated a temporally structured transcriptional defense response. In conclusion, this robust cell culture model of HEV infection provides a powerful tool for studying viral–host interactions that should facilitate the discovery of antiviral drugs for this important zoonotic pathogen.

Published

2020

7. Animal Models for Hepatitis E virus

Author

Laura Corneillie, Dominic H. Banda, and Philip Meuleman

Subjects

CROSS-SPECIES INFECTION, NON-B HEPATITIS, viruses, HEV INFECTION, lcsh:QR1-502, Orthohepevirus, Review, medicine.disease_cause, Virus, lcsh:Microbiology, Viral life cycle, Hepatitis E virus, Virology, vaccine, medicine, Medicine and Health Sciences, Animals, pathogenicity, MONGOLIAN GERBILS, Pathogen, LIVER CHIMERIC MICE, CELL-CULTURE-SYSTEM, biology, GENOTYPE 3, cross-species infection, animal model, Zoonosis, NON-A, Biology and Life Sciences, zoonosis, biology.organism_classification, medicine.disease, WILD RATS, Hepeviridae, Hepatitis E, Disease Models, Animal, Infectious Diseases, AVIAN HEV, Viral hepatitis

Abstract

Hepatitis E virus (HEV) is an underdiagnosed pathogen with approximately 20 million infections each year and currently the most common cause of acute viral hepatitis. HEV was long considered to be confined to developing countries but there is increasing evidence that it is also a medical problem in the Western world. HEV that infects humans belongs to the Orthohepevirus A species of the Hepeviridae family. Novel HEV-like viruses have been observed in a variety of animals and some have been shown to be able to cross the species barrier, causing infection in humans. Several cell culture models for HEV have been established in the past years, but their efficiency is usually relatively low. With the circulation of this virus and related viruses in a variety of species, several different animal models have been developed. In this review, we give an overview of these animal models, indicate their main characteristics, and highlight how they may contribute to our understanding of the basic aspects of the viral life cycle and cross-species infection, the study of pathogenesis, and the evaluation of novel preventative and therapeutic strategies.

Published

2019

8. Human Hepatocyte Transduction with Adeno-Associated Virus Vector.

Author

Song Z, Shao W, Song L, Pei X, and Li C

Subjects

Antibodies, Neutralizing, Genetic Therapy methods, Hepatocytes, Humans, Dependovirus genetics, Genetic Vectors genetics

Abstract

As the adeno-associated virus (AAV) vectors hold unique advantages over other viral vectors, AAV gene therapy has accumulated rapid progress and development. Liver-targeted gene therapy by AAV vectors has been successfully applied in clinical trials for many diseases. Low transduction efficiency and high prevalence of neutralizing antibodies (Nabs), however, are the major obstacles to further translate this therapeutic strategy into clinical trials. Pre-clinical evaluation on hepatocytes could help to elucidate the tropism of AAV serotypes for liver-targeted gene therapy, and could also provide a test model to develop novel AAV mutants with Nabs evasion and high liver tropism. Here, we described the basic laboratory procedure to apply the AAV vector to transduce human hepatocytes in vitro and in vivo with some tips gained from our own experience., (© 2022. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2022

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

Author

Linda Andrus, Ankit Bhatta, Michiel C. Mommersteeg, Eleftherios Michailidis, Charles M. Rice, Anuradha Krishnan, Ype P. de Jong, Koen Vercauteren, Amir Shlomai, Michael Charlton, Eva Billerbeck, Luis Chiriboga, Jing W. Xiao, and Marcus Dorner

Subjects

0301 basic medicine, Hepatitis B virus, Hepatitis C virus, Xenotransplantation, medicine.medical_treatment, Mice, SCID, Biology, medicine.disease_cause, Virus, Monocytes, Natural killer cell, 03 medical and health sciences, Mice, Immune system, medicine, Animals, Humans, Human immune cells, Hepatology, Gastroenterology & Hepatology, 1103 Clinical Sciences, Hepatitis B, medicine.disease, Virology, Killer Cells, Natural, 030104 developmental biology, medicine.anatomical_structure, Immunology, Hepatocytes, Viral hepatitis, Liver chimeric mice

Abstract

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.

Published

2016