A novel humanized mouse model with significant improvement of class-switched, antigen-specific antibody production

Yu, Hua; Borsotti, Chiara; Schickel, Jean-Nicolas; Zhu, Shu; Strowig, Till; Eynon, Elizabeth E.; Frleta, Davor; Gurer, Cagan; Murphy, Andrew; Yancopouloš, George D.; Meffre, Eric; Manz, Markus G.; Flavell, Richard A.

doi:10.1182/blood-2016-04-709584

Cited by 102 publications

(105 citation statements)

References 42 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The addition of human Il6 gene knock‐in has demonstrated improved haematopoiesis, class switching and a high frequency of somatic hypermutation …”

Section: Humoral Immunity In Humanized Micementioning

confidence: 99%

“…15,59 The addition of human Il6 gene knock-in has demonstrated improved haematopoiesis, class switching and a high frequency of somatic hypermutation. 26 Due to this, a further advancement of the MISTRG mouse was created, with the addition of the human Il6 by gene knock-in, resulting in the new MISTRG-6 strain. 26 This new model shows improved B-cell and malignant plasma cell development, to investigate their effects on lytic bone disease, however, this strain is yet to be used in the context of infectious disease.…”

Section: Humoral Immunity In Humanized Micementioning

confidence: 99%

See 1 more Smart Citation

A Hitchhiker's guide to humanized mice: new pathways to studying viral infections

2018

View full text Add to dashboard Cite

SummaryHumanized mice are increasingly appreciated as an incredibly powerful platform for infectious disease research. The often very narrow species tropism of many viral infections, coupled with the sometimes misleading results from preclinical studies in animal models further emphasize the need for more predictive model systems based on human cells rather than surrogates. Humanized mice represent such a model and have been greatly enhanced with regards to their immune system reconstitution as well as immune functionality in the past years, resulting in their recommendation as a preclinical model by the US Food and Drug Administration. This review aims to give a detailed summary of the generation of human peripheral blood lymphocyte‐, CD34+ haematopoietic stem cell‐ and bone marrow/liver/thymus‐reconstituted mice and available improved models (e.g. myeloid‐ or T‐cell‐only mice, MISTRG, NSG‐SGM3). Additionally, we summarize human‐tropic viral infections, for which humanized mice offer a novel approach for the study of disease pathogenesis as well as future perspectives for their use in biomedical, drug and vaccine research.

show abstract

“…The addition of human Il6 gene knock‐in has demonstrated improved haematopoiesis, class switching and a high frequency of somatic hypermutation …”

Section: Humoral Immunity In Humanized Micementioning

confidence: 99%

Section: Humoral Immunity In Humanized Micementioning

confidence: 99%

A Hitchhiker's guide to humanized mice: new pathways to studying viral infections

2018

View full text Add to dashboard Cite

show abstract

“…Studies using sera from DENV immunized IL6 transgenic BLT NSG mice also showed improved IgG responses compared to BLT NSG mice (unpublished data). A recent report suggests that IL6 knock-in mice had improved class-switched memory B cells and ovalbumin specific IgG in response to immunization with OVA [35]. …”

Section: Improving B Cell and Antibody Responses In Humanized Blt Nsgmentioning

confidence: 99%

Humanized mouse models to study human cell-mediated and humoral responses to dengue virus

Mathew

2017

Current Opinion in Virology

View full text Add to dashboard Cite

Several candidate dengue virus vaccines are in clinical trials and show promise as an effective measure to control dengue. However, it is becoming clear that additional vaccine candidates may be needed as there is concern about the durability of the immune response to all four serotypes of vaccine components and efficacy varies dependent on the immune status of the individual. The lack of an appropriate animal model to mimic human dengue has deterred the development of vaccines and anti-viral therapies to dengue virus. The focus of this review is to discuss advances in the development of humanized animal models and to highlight how they could be used for antiviral and dengue vaccine testing if limitations with cell-mediated immunity and seroconversion to IgG are overcome.

show abstract

“…Thus, mice expressing human cytokines, including a combination of SCF, GM-CSF, and IL-3 (NSG-SGM3) or M-CSF, IL-3, GM-CSF, and thrombopoietin (MISTRG) show improved myelopoiesis 7, 8 . Mice carrying a knock-in of human IL-6 show improved B-cell development and function 9 .…”

Section: Introductionmentioning

confidence: 99%

Enhanced differentiation of functional human T cells in NSGW41 mice with tissue-specific expression of human interleukin-7

Coppin

Sundarasetty

Rahmig

et al. 2020

Preprint

View full text Add to dashboard Cite

Key points 411.Increased intrathymic human T cell differentiation in the absence of 42 pathological lymphoproliferation in humanized NSGW41hIL7 mice. 43 44 2.Increased peripheral human T cell populations in NSGW41hIL7 mice making 45 the analysis of human regulatory T cells in vivo feasible. 46 47 48 49 50 Abstract 51Humanized mouse models have become increasingly valuable tools to study human 52 hematopoiesis and infectious diseases. However, human T cell differentiation 53 remains inefficient. We generated mice expressing human interleukin (IL-7), a critical 54 growth and survival factor for T cells, under the control of murine IL-7 regulatory 55 elements. After transfer of human cord blood-derived hematopoietic stem and 56 progenitor cells, transgenic mice on the NSGW41 background, termed 57NSGW41hIL7, showed elevated and prolonged human cellularity in the thymus while 58 maintaining physiological ratios of thymocyte subsets. As a consequence, numbers 59 of functional human T cells in the periphery were increased without evidence for 60 pathological lymphoproliferation or aberrant expansion of effector or memory-like T 61 cells. We conclude that the novel NSGW41hIL7 strain represents an optimized 62 mouse model for humanization to better understand human T cell differentiation in 63 vivo and to generate a human immune system with a better approximation of human 64 lymphocyte ratios. 65 knock-in of hIL-7 and hIL-15 on the NSG background displayed massive skewing 131 towards CD8 SP cells at the expense of DP thymocytes 17 , suggesting that tissue-132 specific expression of human cytokines alone is insufficient to promote human T cell

show abstract

A novel humanized mouse model with significant improvement of class-switched, antigen-specific antibody production

Cited by 102 publications

References 42 publications

A Hitchhiker's guide to humanized mice: new pathways to studying viral infections

A Hitchhiker's guide to humanized mice: new pathways to studying viral infections

Humanized mouse models to study human cell-mediated and humoral responses to dengue virus

Enhanced differentiation of functional human T cells in NSGW41 mice with tissue-specific expression of human interleukin-7

Contact Info

Product

Resources

About