Literature DB >> 8243828

Lymph node T-cells do not optimally transfer diabetes in NOD mice.

F Lepault1, C Faveeuw, J J Luan, M C Gagnerault.   

Abstract

The nonobese diabetic mouse in a model of spontaneous development of autoimmune type I diabetes. The disease can be induced in young, irradiated recipients by injecting splenic T-cells from diabetic donors. The adoptive transfer of diabetes requires the presence of both CD4+ and CD8+ splenic T-cell subsets. To test whether diabetogenic cells distribute in other lymphoid organs of diabetic mice, we first analyzed lymph node cells. Lymph node cells were much less efficient in transferring diabetes than splenocytes. This inefficacious transfer was not attributable to the absence of hematopoietic precursors or a lack of macrophages. Lymph node cells did not protect from the transfer of diabetes by splenocytes, indicating the absence of suppressor cells. Although CD8+ lymph node T-cells seemed functionally comparable to CD8+ splenocytes, CD4+ lymph node T-cells failed to cooperate with CD8+ splenocytes to transfer diabetes. Our study suggests that diabetogenic cells are not evenly distributed in the different lymphoid organs. This may reflect a differential migration pattern of pathogenic T-cells in this animal model.

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Year:  1993        PMID: 8243828     DOI: 10.2337/diab.42.12.1823

Source DB:  PubMed          Journal:  Diabetes        ISSN: 0012-1797            Impact factor:   9.461


  2 in total

1.  Low CD25 on autoreactive Tregs impairs tolerance via low dose IL-2 and antigen delivery.

Authors:  Chie Hotta-Iwamura; Charles Benck; William D Coley; Yi Liu; Yongge Zhao; Juan A Quiel; Kristin V Tarbell
Journal:  J Autoimmun       Date:  2018-02-10       Impact factor: 7.094

2.  Pancreatic lymph nodes are required for priming of beta cell reactive T cells in NOD mice.

Authors:  Marie-Claude Gagnerault; Jian Jian Luan; Chantal Lotton; Françoise Lepault
Journal:  J Exp Med       Date:  2002-08-05       Impact factor: 14.307

  2 in total

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