Journal article

Disabling an integral CTL epitope allows suppression of autoimmune diabetes by intranasal proinsulin peptide

NR Martinez, P Augstein, AK Moustakas, GK Papadopoulos, S Gregori, L Adorini, DC Jackson, LC Harrison

Journal of Clinical Investigation | AMER SOC CLINICAL INVESTIGATION INC | Published : 2003

DOI: 10.1172/JCI200317166

Abstract

Insulin is a major target of the autoimmune response associated with destruction of pancreatic β cells in type 1 diabetes. A peptide that spans the junction of the insulin B chain and the connecting (C) peptide in proinsulin has been reported to stimulate T cells from humans at risk for type 1 diabetes and autoimmune diabetes-prone NOD mice. Here we show that proinsulin B24-C36 peptide binds to I-Ag7, the MHC class II molecule of the NOD mouse, and, after intranasal administration, induces regulatory CD4+ T cells that, in the absence of CD8+ T cells, block the adoptive transfer of diabetes. Curiously, however, intranasal B24-C36 did not inhibit development of spontaneous diabetes in treated ..

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Keywords

Autoantigen
Mhc Class-I
Beta-Cell Function
Disease
Vaccine Related
Immunization
Immunotherapy
Medicine, Research & Experimental
Molecule
32 Biomedical and Clinical Sciences
T-Cells
Research & Experimental Medicine
Autoimmune Disease
Life Sciences & Biomedicine
Nod Mice
Tolerance
Science & Technology
Myelin Basic-Protein
Metabolic and Endocrine
Oral Insulin
Diabetes
3204 Immunology