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    Human BLyS facilitates engraftment of human PBL derived B cells in immunodeficient mice

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    Authors
    Schmidt, Madelyn R.
    Appel, Michael C.
    Giassi, Lisa J.
    Greiner, Dale L.
    Shultz, Leonard D.
    Woodland, Robert T.
    UMass Chan Affiliations
    Department of Medicine, Division of Diabetes
    Department of Molecular Genetics and Microbiology
    Graduate School of Biomedical Sciences
    Document Type
    Journal Article
    Publication Date
    2008-09-12
    Keywords
    Animals; Antigens, CD19; B-Lymphocytes; Cell Nucleus; Cell Separation; Flow Cytometry; Humans; Mice; Mice, Inbred NOD; Mice, SCID; NF-kappa B; Pneumococcal Vaccines; Receptors, Tumor Necrosis Factor; Recombinant Proteins; Signal Transduction
    Life Sciences
    Medicine and Health Sciences
    
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    Abstract
    The production of fully immunologically competent humanized mice engrafted with peripheral lymphocyte populations provides a model for in vivo testing of new vaccines, the durability of immunological memory and cancer therapies. This approach is limited, however, by the failure to efficiently engraft human B lymphocytes in immunodeficient mice. We hypothesized that this deficiency was due to the failure of the murine microenvironment to support human B cell survival. We report that while the human B lymphocyte survival factor, B lymphocyte stimulator (BLyS/BAFF) enhances the survival of human B cells ex vivo, murine BLyS has no such protective effect. Although human B cells bound both human and murine BLyS, nuclear accumulation of NF-kappaB p52, an indication of the induction of a protective anti-apoptotic response, following stimulation with human BLyS was more robust than that induced with murine BLyS suggesting a fundamental disparity in BLyS receptor signaling. Efficient engraftment of both human B and T lymphocytes in NOD rag1(-/-) Prf1(-/-) immunodeficient mice treated with recombinant human BLyS is observed after adoptive transfer of human PBL relative to PBS treated controls. Human BLyS treated recipients had on average 40-fold higher levels of serum Ig than controls and mounted a de novo antibody response to the thymus-independent antigens in pneumovax vaccine. The data indicate that production of fully immunologically competent humanized mice from PBL can be markedly facilitated by providing human BLyS.
    Source
    PLoS ONE. 2008 Sep 11;3(9):e3192. Link to article on publisher's site
    DOI
    10.1371/journal.pone.0003192
    Permanent Link to this Item
    http://hdl.handle.net/20.500.14038/33008
    PubMed ID
    18784835; 18784835
    Related Resources
    Link to Article in PubMed
    ae974a485f413a2113503eed53cd6c53
    10.1371/journal.pone.0003192
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    Morningside Graduate School of Biomedical Sciences Scholarly Publications

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