Title of article
A new Hu-PBL model for the study of human islet alloreactivity based on NOD-scid mice bearing a targeted mutation in the IL-2 receptor gamma chain gene
Author/Authors
King، نويسنده , , Marie and Pearson، نويسنده , , Todd and Shultz، نويسنده , , Leonard D. and Leif، نويسنده , , Jean and Bottino، نويسنده , , Rita and Trucco، نويسنده , , Massimo and Atkinson، نويسنده , , Mark A. and Wasserfall، نويسنده , , Clive and Herold، نويسنده , , Kevan C. and Woodland، نويسنده , , Robert T. and Schmidt، نويسنده , , Madelyn R. and Woda، نويسنده , , Bruce A. and Thompson، نويسنده , , Mic، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2008
Pages
12
From page
303
To page
314
Abstract
Immunodeficient NOD-scid mice bearing a targeted mutation in the IL2 receptor common gamma chain (Il2rγnull) readily engraft with human stem cells. Here we analyzed human peripheral blood mononuclear cells (PBMC) for their ability to engraft NOD-scid Il2rγnull mice and established engraftment kinetics, optimal cell dose, and the influence of injection route. Even at low PBMC input, NOD-scid Il2rγnull mice reproducibly support high human PBMC engraftment that plateaus within 3–4 weeks. In contrast to previous stocks of immunodeficient mice, we observed low intra- and inter-donor variability of engraftment. NOD-scid Il2rγnull mice rendered hyperglycemic by streptozotocin treatment return to normoglycemia following transplantation with human islets. Interestingly, these human islet grafts are rejected following injection of HLA-mismatched human PBMC as evidenced by return to hyperglycemia and loss of human C-peptide. These data suggest that humanized NOD-scid Il2rγnull mice may represent an important surrogate for investigating in vivo mechanisms of human islet allograft rejection.
Keywords
rejection , Hu-PBL-scid , mouse , human , NOD-scid , scid , IL-2r gamma chain , Transplantation , Islet , Humanized mice
Journal title
Clinical Immunology
Serial Year
2008
Journal title
Clinical Immunology
Record number
1852910
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