Abstract

Type 1 diabetes (T1D) is an autoimmune disease associated with T-cell mediated destruction of insulin- producing ?-cells. Prediabetic individuals typically lose tolerance first to insulin followed by other islet auto- antigens. This repeated, sequential loss of tolerance suggests that local antigenic responses may be skewed in T1D in ways that contribute to the loss of tolerance. We recently identified characteristic changes in the pancreatic lymph nodes (PLN) of individuals with T1D. Specifically, hyaluronan (HA), an extracellular matrix polymer, is abundant within the inter-follicular regions of PLN ? the tissue sites where T-cell responses to self-antigens are primed ? of cadaveric donors with T1D. Intrigued by these exciting results, we investigated the possibility that HA may play a role in loss of immune tolerance by potentiating the immune synapse between dendritic cells (DC) and T-cells. We find that activated, mature DC generate a ?coat? of HA in association with hyaluronan synthase 3 (HAS3) that modulates antigen presentation, enhancing T-cell activation and proliferation in response to otherwise weak antigenic signals. Conversely, treatments that clear HA or disrupt its binding to CD44 (hyaluronidase, CD44 blocking antibodies, or 4-methylumbelliferone (4-MU), an HA synthesis inhibitor), reduce the efficiency of antigen presentation and promote peripheral FoxP3+ regulatory T-cells (Treg) induction. These data suggest a model whereby interactions between HA surrounding the DC and CD44 on T-cells stabilize the immune synapse. This stabilization, in turn, increases the effective affinity of TCR-MHC interactions, increasing positive selection of otherwise low affinity, autoreactive T-cells. This hypothesis, if true, represents a novel mechanism of co-stimulation of T-cells that contributes to the loss of immune tolerance in T1D. It may be possible to target HA therapeutically to promote tolerance. We recently reported that treatment with oral 4-MU prevented T1D and promoted Foxp3+ Treg expansion in multiple mouse models of T1D. These results are particularly exciting because 4-MU is already an approved drug, currently used for a different indication in children and adults. It may be possible to repurpose 4-MU to prevent T1D in at-risk subjects. However, it is essential that we first establish how HA promotes autoimmunity. We hypothesize that pericellular HA surrounding DC contributes to priming of autoreactive T-cells in T1D. To test this hypothesis, in Aim 1, we will determine how pericellular HA on DC impacts immune synapse formation with T-cells.
In Aim 2, we will elucidate how pericellular HA on DC contributes to the loss of tolerance in autoimmune diabetes. Finally, in Aim 3, we will determine whether the appearance of HA within PLN coincides with the loss of tolerance in human prediabetes and the role of DC pericellular HA in mediating T-cell responses. Together, these studies will yield novel insights into the fundamental mechanisms underlying antigen presentation and the development of autoimmunity as well as a potentially transformative therapy for T1D.

Public Health Relevance

Type 1 diabetes (T1D) results when the body's own immune system destroys insulin-producing ?-cells. We have identified hallmark changes in the lymph nodes of people with T1D that we believe may contribute to this loss of immune tolerance to ?-cell self-antigens. Here, we propose to investigate how the tissue microenvi- ronment within lymph nodes contributes to antigen presentation and to the loss of immune tolerance in T1D.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK096087-07A1
Application #
9594122
Study Section
Hypersensitivity, Autoimmune, and Immune-mediated Diseases Study Section (HAI)
Program Officer
Spain, Lisa M
Project Start
2012-09-01
Project End
2022-08-31
Budget Start
2018-09-17
Budget End
2019-08-31
Support Year
7
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94304

  Publications

Nagy, Nadine; de la Zerda, Adi; Kaber, Gernot et al. (2018) Hyaluronan content governs tissue stiffness in pancreatic islet inflammation. J Biol Chem 293:567-578
Nagy, Nadine; Sunkari, Vivekananda G; Kaber, Gernot et al. (2018) Hyaluronan levels are increased systemically in human type 2 but not type 1 diabetes independently of glycemic control. Matrix Biol :
Medina, Carlos O; Nagy, Nadine; Bollyky, Paul L (2018) Extracellular matrix and the maintenance and loss of peripheral immune tolerance in autoimmune insulitis. Curr Opin Immunol 55:22-30
Nagy, Nadine; Kuipers, Hedwich F; Marshall, Payton L et al. (2018) Hyaluronan in immune dysregulation and autoimmune diseases. Matrix Biol :
Homann, Susanne; Grandoch, Maria; Kiene, Lena S et al. (2018) Hyaluronan synthase 3 promotes plaque inflammation and atheroprogression. Matrix Biol 66:67-80
Kuipers, Hedwich F; Yoon, Jane; van Horssen, Jack et al. (2017) Phosphorylation of ?B-crystallin supports reactive astrogliosis in demyelination. Proc Natl Acad Sci U S A 114:E1745-E1754
Balaji, Swathi; Wang, Xinyi; King, Alice et al. (2017) Interleukin-10-mediated regenerative postnatal tissue repair is dependent on regulation of hyaluronan metabolism via fibroblast-specific STAT3 signaling. FASEB J 31:868-881
Gebe, John A; Yadava, Koshika; Ruppert, Shannon M et al. (2017) Modified High-Molecular-Weight Hyaluronan Promotes Allergen-Specific Immune Tolerance. Am J Respir Cell Mol Biol 56:109-120
Kuipers, H F; Nagy, N; Ruppert, S M et al. (2016) The pharmacokinetics and dosing of oral 4-methylumbelliferone for inhibition of hyaluronan synthesis in mice. Clin Exp Immunol 185:372-81
Kuipers, Hedwich F; Rieck, Mary; Gurevich, Irina et al. (2016) Hyaluronan synthesis is necessary for autoreactive T-cell trafficking, activation, and Th1 polarization. Proc Natl Acad Sci U S A 113:1339-44

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