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Publication : Shared TCR Vbeta gene expression by the pancreas and salivary gland in immunodeficient alymphoplasic mice.

First Author  Yamamichi M Year  1997
Journal  J Immunol Volume  159
Issue  1 Pages  427-32
PubMed ID  9200482 Mgi Jnum  J:41579
Mgi Id  MGI:894066 Doi  10.4049/jimmunol.159.1.427
Citation  Yamamichi M, et al. (1997) Shared TCR Vbeta gene expression by the pancreas and salivary gland in immunodeficient alymphoplasic mice. J Immunol 159(1):427-32
abstractText  Mice with the homozygous mutation alymphoplasia (aly) lack lymph nodes and Peyer's patches and show defects in both humoral and cellular immunity. In these mice, spontaneous infiltration of mononuclear cells was observed in multiple exocrine organs, including the pancreas, salivary glands, and lacrimal glands from the age of 15 wk, progressing to a marked tissue destruction at the age of 25 wk, Using this strain, we examined the phenotypes and TCR V beta gene expression of infiltrating T cells to identify the pathologic role of T cell immunity in idiopathic pancreatitis, Most of the infiltrating cells were CD4(+) and Thy-1(+) cells. Analysis of the TCR gene expression on T cells infiltrating the pancreas and salivary glands showed a high expression of V beta 1 and V beta 5 in both organs at the age of 15 wk, In contrast, a diverse expression of TCR V beta genes was noted at 25 wk, Sequence analysis of complementarity-determining region 3 (CDR3) of the most prominent TCR V beta gene family expressed in these cells, V beta 1, showed oligoclonal expansion of infiltrating T cells in both organs, Frequent use of glutamine and proline at position 97 was observed in paired tissues, Our data suggest that oligoclonal expansion of organ specific T cells might be one of the etiologic mechanisms of chronic pancreatitis and that common autoantigens could trigger autoimmunity in multiple organs.
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