Abstract
Type 1 diabetes (T1D) is a T cell-mediated disease. It is strongly associated with susceptibility haplotypes within the major histocompatibility complex, but this association accounts for an estimated 50% of susceptibility. Other studies have identified as many as 50 additional susceptibility loci, but the effect of most is very modest (odds ratio (OR) <1.5). What accounts for the “missing heritability” is unknown and is often attributed to environmental factors. Here we review new data on the cognate ligand of MHC molecules, the T cell receptor (TCR). In rats, we found that one allele of a TCR variable gene, Vβ13A, is strongly associated with T1D (OR >5) and that deletion of Vβ13+ T cells prevents diabetes. A role for the TCR is also suspected in NOD mice, but TCR regions have not been associated with human T1D. To investigate this disparity, we tested the hypothesis in silico that previous studies of human T1D genetics were underpowered to detect MHC-contingent TCR susceptibility. We show that stratifying by MHC markedly increases statistical power to detect potential TCR susceptibility alleles. We suggest that the TCR regions are viable candidates for T1D susceptibility genes, could account for “missing heritability,” and could be targets for prevention.
Highlights
Type 1 diabetes (T1D) is a T cell-mediated autoimmune disease that afflicts a million persons in the USA [1, 2]
To examine the possibility of germ-line human T cell receptor (TCR) variants having a functional impact on the immune repertoire and a potential impact on autoimmunity and T1D in particular, we extended the analysis of polymorphism in TRBV and compiled a comprehensive set of nonsynonymous polymorphisms in the human TRAV and TRBV genes in regions known to contact the pMHC (Table 2) [56]
We examined this contention further using a dataset of TRAV and TRBV single nucleotide polymorphism (SNP) downloaded from the UCSC genome browser [58], selecting only SNPs found within TRAV and TRBV exons from IMGT reference sequences [55]
Summary
Type 1 diabetes (T1D) is a T cell-mediated autoimmune disease that afflicts a million persons in the USA [1, 2]. It is a polygenic disorder resulting from the interaction of multiple gene variants [3] and environmental factors [4]. Predictions of T1D, incorporating both HLA and all currently known loci, generate a λs of only 5 [3, 15], a recently reported strategy based on combining multiple risk alleles appears to hold promise [16]
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