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HLA-B*39:06 Efficiently Mediates Type 1 Diabetes in a Mouse Model Incorporating Reduced Thymic Insulin Expression

View ORCID ProfileJennifer Schloss, View ORCID ProfileRiyasat Ali, Jeremy J Racine, Harry Chapman, David Serreze, View ORCID ProfileTeresa DiLorenzo
doi: https://doi.org/10.1101/264531
Jennifer Schloss
Albert Einstein College of Medicine;
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Riyasat Ali
Albert Einstein College of Medicine;
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Jeremy J Racine
The Jackson Laboratory
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Harry Chapman
The Jackson Laboratory
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David Serreze
The Jackson Laboratory
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Teresa DiLorenzo
Albert Einstein College of Medicine;
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  • For correspondence: teresa.dilorenzo@einstein.yu.edu
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Abstract

Type 1 diabetes (T1D) is characterized by T cell-mediated destruction of the insulin-producing β cells of the pancreatic islets. Among the loci associated with T1D risk, those most predisposing are found in the MHC region. HLA-B*39:06 is the most predisposing class I MHC allele and is associated with an early age of onset. To establish an NOD mouse model for the study of HLA-B*39:06, we expressed it in the absence of murine class I MHC. HLA-B*39:06 was able to mediate the development of CD8 T cells, support lymphocytic infiltration of the islets, and confer T1D susceptibility. Because reduced thymic insulin expression is associated with increased T1D risk in patients, we incorporated this in our model as well, finding that HLA-B*39:06-transgenic NOD mice with reduced thymic insulin expression have an earlier age of disease onset and a higher overall prevalence as compared to littermates with typical thymic insulin expression. This was despite virtually indistinguishable blood insulin levels, T cell subset percentages, and TCR Vβ family usage, indicating that reduced thymic insulin expression does not impact T cell development on a global scale. Rather, we propose that it allows the thymic escape of insulin-reactive HLA-B*39:06-restricted T cells which participate in β cell destruction. We also found that in mice expressing either HLA-B*39:06 or HLA-A*02:01 in the absence of murine class I MHC, HLA transgene identity alters TCR Vβ usage, which may contribute to varying diabetogenic CD8 T cell repertoires in the presence of different HLA class I alleles.

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Posted February 13, 2018.
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HLA-B*39:06 Efficiently Mediates Type 1 Diabetes in a Mouse Model Incorporating Reduced Thymic Insulin Expression
Jennifer Schloss, Riyasat Ali, Jeremy J Racine, Harry Chapman, David Serreze, Teresa DiLorenzo
bioRxiv 264531; doi: https://doi.org/10.1101/264531
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HLA-B*39:06 Efficiently Mediates Type 1 Diabetes in a Mouse Model Incorporating Reduced Thymic Insulin Expression
Jennifer Schloss, Riyasat Ali, Jeremy J Racine, Harry Chapman, David Serreze, Teresa DiLorenzo
bioRxiv 264531; doi: https://doi.org/10.1101/264531

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