Entry of diabetogenic T cells into islets induces changes that lead to amplification of the cellular response

B Calderon, JA Carrero, MJ Miller… - Proceedings of the …, 2011 - National Acad Sciences
B Calderon, JA Carrero, MJ Miller, ER Unanue
Proceedings of the National Academy of Sciences, 2011National Acad Sciences
In an accompanying paper, we find specific localization of diabetogenic T cells only to islets
of Langerhans bearing the specific antigen. Instrumental in the specific localization was the
presence of intraislet dendritic cells bearing the β-cell-peptide-MHC complex. Here, we
report that the entry of diabetogenic CD4 T cells very rapidly triggered inflammatory gene
expression changes in islets and vessels by up-regulating chemokines and adhesion
molecules. Vascular cell adhesion molecule-1 (VCAM-1) expression was notable in blood …
In an accompanying paper, we find specific localization of diabetogenic T cells only to islets of Langerhans bearing the specific antigen. Instrumental in the specific localization was the presence of intraislet dendritic cells bearing the β-cell-peptide-MHC complex. Here, we report that the entry of diabetogenic CD4 T cells very rapidly triggered inflammatory gene expression changes in islets and vessels by up-regulating chemokines and adhesion molecules. Vascular cell adhesion molecule-1 (VCAM-1) expression was notable in blood vessels, as was intercellular adhesion molecule-1 (ICAM-1). ICAM-1 was also found on β-cells. These expression changes induced the entry of nonspecific T cells that otherwise did not localize to the islets. In contrast to the entry of diabetogenic CD4 T cells, the entrance of nonspecific T cells required a chemokine response and VCAM-1 expression by the islets. IFN-γ was important for the early gene expression changes in the islets. By microarray analysis, we detected up-regulation of a group of IFN-inducible genes as early as 8 h post–T-cell transfer. These studies establish that entry of diabetogenic T cells induces a state of receptivity of islets to subsequent immunological insults.
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