Abstract

For many autoimmune diseases new classes of biologic therapies have proven beneficial. These novel drugs that alleviate damaging inflammation were developed based on a deep understanding of the specific immune proteins (predominantly cytokines or cell membrane proteins) that cause disease pathology. To date, we lack such a sophisticated understanding of factors that cause type 1 diabetes (T1D) pathology; however, our knowledge is evolving as new discoveries shed light on mechanisms of T1D. For example, type 1 interferons (IFN1) are a family of cytokines that play a key role T1D where they impair ?-cell function, enhance immune- surveillance, and augment CD8+ cytolytic T cell (CTL) mediated ?-cell killing. IFN1 represent a key connection between immune dysregulation, ?-cell dysfunction, genes that form disease susceptibility, and environmental factors (i.e., danger signals) that collectively modulate T1D development. What is still lacking is a fundamental understanding of how IFN1 responses go awry in T1D and thus what types of interventions would be useful. This project will focus on dissecting the complex genetics of T1D to clarify mechanisms of IFN1-induced pathogenesis. At least seven T1D risk genes are involved in IFN1 production or signaling pathways (IFIH1, TYK2, SOCS1, STAT4, PTPN2, PTPN22, and IL10). Two of these genes, IFIH1 and TYK2, have coding variants that are associated with T1D risk. Hence, these genes are excellent targets for genotype:phenotype studies. IFN-induced with helicase C domain 1 (IFIH1) is a cytoplasmic protein that binds to viral RNA structures upon infection, triggering downstream signaling to elicit IFN1 production. How IFIH1 coding variants affect responses by ?-cells or immune cells (with Project 2) to self- or viral-RNA molecules will be the focus of Aim 1. Previous studies have identified a P1104A coding variant in TYK2 as associated with protection against T1D. Like IFIH1 variants, this TYK2 allotype alters IFN1 signaling in immune cells and could impact IFN1 signaling in islet cells. How the TYK2 variant affects ?-cell (with Project 2) or immune cell responses (with Project 3) to IFN1 will be the focus of Aim 2. We predict that IFIH1 risk variants are excessively sensitive to self-RNA species or short viral dsRNA. We also predict that TYK2 risk variants allow maximal IFN1 induced signaling leading to IFN-induced ?-cell failure or IFN-induced CTL effector function. We hypothesize that risk alleles of IFIH1 and TYK2 improperly integrate responses to cellular danger signals, leading to immune dysregulation and T1D onset. This project will utilize an extensive repository of deeply genotyped T1D and control donor cells as well as induced pluripotent stem cells (iPSCs), to interrogate precise questions surrounding how mechanisms of innate immune sensing and IFN1 production lead to ?-cell loss in T1D. These studies are highly synergistic with Projects 2 & 3 are will rely heavily of Cores A & B for successful completion.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI042288-22
Application #
9944324
Study Section
Special Emphasis Panel (ZAI1)
Project Start
1997-09-30
Project End
2023-05-31
Budget Start
2020-06-01
Budget End
2021-05-31
Support Year
22
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Florida
Department
Type
DUNS #
969663814
City
Gainesville
State
FL
Country
United States
Zip Code
32611

  Publications

Perry, Daniel J; Wasserfall, Clive H; Oram, Richard A et al. (2018) Application of a Genetic Risk Score to Racially Diverse Type 1 Diabetes Populations Demonstrates the Need for Diversity in Risk-Modeling. Sci Rep 8:4529
Chen, Yi-Guang; Mathews, Clayton E; Driver, John P (2018) The Role of NOD Mice in Type 1 Diabetes Research: Lessons from the Past and Recommendations for the Future. Front Endocrinol (Lausanne) 9:51
Kusmartseva, Irina; Beery, Maria; Philips, Tiffany et al. (2018) Hospital time prior to death and pancreas histopathology: implications for future studies. Diabetologia 61:954-958
Hu, Ronghua; Xia, Chang-Qing; Butfiloski, Edward et al. (2018) Effect of high glucose on cytokine production by human peripheral blood immune cells and type I interferon signaling in monocytes: Implications for the role of hyperglycemia in the diabetes inflammatory process and host defense against infection. Clin Immunol 195:139-148
Smith, Mia J; Rihanek, Marynette; Wasserfall, Clive et al. (2018) Loss of B-Cell Anergy in Type 1 Diabetes Is Associated With High-Risk HLA and Non-HLA Disease Susceptibility Alleles. Diabetes 67:697-703
Whitener, Robert L; Gallo Knight, Lisa; Li, Jianwei et al. (2017) The Type 1 Diabetes-Resistance Locus Idd22 Controls Trafficking of Autoreactive CTLs into the Pancreatic Islets of NOD Mice. J Immunol 199:3991-4000
Wang, Qiming; Racine, Jeremy J; Ratiu, Jeremy J et al. (2017) Transient BAFF Blockade Inhibits Type 1 Diabetes Development in Nonobese Diabetic Mice by Enriching Immunoregulatory B Lymphocytes Sensitive to Deletion by Anti-CD20 Cotherapy. J Immunol 199:3757-3770
Yeh, Wen-I; Seay, Howard R; Newby, Brittney et al. (2017) Avidity and Bystander Suppressive Capacity of Human Regulatory T Cells Expressing De Novo Autoreactive T-Cell Receptors in Type 1 Diabetes. Front Immunol 8:1313
Campbell-Thompson, Martha L; Atkinson, Mark A; Butler, Alexandra E et al. (2017) Re-addressing the 2013 consensus guidelines for the diagnosis of insulitis in human type 1 diabetes: is change necessary? Diabetologia 60:753-755
Wallet, Mark A; Santostefano, Katherine E; Terada, Naohiro et al. (2017) Isogenic Cellular Systems Model the Impact of Genetic Risk Variants in the Pathogenesis of Type 1 Diabetes. Front Endocrinol (Lausanne) 8:276

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