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FOXP3+ regulatory T cells use heparanase to access IL-2 bound to ECM in inflamed tissues

Hunter A. Martinez, Ievgen Koliesnik, Gernot Kaber, Jacqueline K. Reid, Nadine Nagy, Graham Barlow, Ben A. Falk, Carlos O. Medina, Aviv Hargil, Israel Vlodavsky, Jin-Ping Li, Magdiel Pérez-Cruz, Sai-Wen Tang, Everett H. Meyer, Lucile E. Wrenshall, James D. Lord, K. Christopher Garcia, Theo D. Palmer, Lawrence Steinman, Gerald T. Nepom, Thomas N. Wight, Paul L. Bollyky, Hedwich F. Kuipers
doi: https://doi.org/10.1101/2023.02.26.529772
Hunter A. Martinez
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Ievgen Koliesnik
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Gernot Kaber
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Jacqueline K. Reid
2Department of Clinical Neurosciences, Cumming School of Medicine, University of Calgary; Calgary, Canada
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Nadine Nagy
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Graham Barlow
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Ben A. Falk
3Matrix Biology Program, Benaroya Research Institute; Seattle, USA
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Carlos O. Medina
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Aviv Hargil
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Israel Vlodavsky
4Tumor Integrated Cancer Center, Technion-Israel Institute of Technology; Haifa, Israel
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Jin-Ping Li
5Department of Medical Biochemistry and Microbiology, Uppsala University; Uppsala, Finland
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Magdiel Pérez-Cruz
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Sai-Wen Tang
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Everett H. Meyer
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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Lucile E. Wrenshall
6Department of Surgery, Boonshoft School of Medicine, Wright State University; Dayton, USA
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James D. Lord
7Translational Research Program, Benaroya Research Institute; Seattle, USA
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K. Christopher Garcia
8Department of Molecular & Cellular Physiology, Stanford University; Stanford, USA
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Theo D. Palmer
9Department of Neurosurgery, Stanford University School of Medicine; Stanford, USA
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Lawrence Steinman
10Department of Neurology and Neurological Sciences, Stanford University School of Medicine; Stanford, USA
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Gerald T. Nepom
11Immune Tolerance Network, Benaroya Research Institute; Seattle, USA
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Thomas N. Wight
3Matrix Biology Program, Benaroya Research Institute; Seattle, USA
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Paul L. Bollyky
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
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  • For correspondence: hedwich.kuipers@ucalgary.ca
Hedwich F. Kuipers
1Department of Medicine, Stanford University School of Medicine; Stanford, USA
2Department of Clinical Neurosciences, Cumming School of Medicine, University of Calgary; Calgary, Canada
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  • For correspondence: hedwich.kuipers@ucalgary.ca
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Abstract

FOXP3+ regulatory T cells (Treg) depend on exogenous IL-2 for their survival and function, but circulating levels of IL-2 are low, making it unclear how Treg access this critical resource in vivo. Here, we show that Treg use heparanase (HPSE) to access IL-2 sequestered by heparan sulfate (HS) within the extracellular matrix (ECM) of inflamed central nervous system tissue. HPSE expression distinguishes human and murine Treg from conventional T cells and is regulated by the availability of IL-2. HPSE-/- Treg have impaired stability and function in vivo, including the experimental autoimmune encephalomyelitis (EAE) mouse model of multiple sclerosis. Conversely, endowing Treg with HPSE enhances their ability to access HS-sequestered IL-2 and their tolerogenic function in vivo. Together, these data identify novel roles for HPSE and the ECM in immune tolerance, providing new avenues for improving Treg-based therapy of autoimmunity.

One-Sentence Summary Regulatory T cells use heparanase to strip IL-2 bound to extracellular matrix within inflamed tissues, thereby supporting their homeostasis and function.

Competing Interest Statement

The authors have declared no competing interest.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
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Posted February 27, 2023.
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FOXP3+ regulatory T cells use heparanase to access IL-2 bound to ECM in inflamed tissues
Hunter A. Martinez, Ievgen Koliesnik, Gernot Kaber, Jacqueline K. Reid, Nadine Nagy, Graham Barlow, Ben A. Falk, Carlos O. Medina, Aviv Hargil, Israel Vlodavsky, Jin-Ping Li, Magdiel Pérez-Cruz, Sai-Wen Tang, Everett H. Meyer, Lucile E. Wrenshall, James D. Lord, K. Christopher Garcia, Theo D. Palmer, Lawrence Steinman, Gerald T. Nepom, Thomas N. Wight, Paul L. Bollyky, Hedwich F. Kuipers
bioRxiv 2023.02.26.529772; doi: https://doi.org/10.1101/2023.02.26.529772
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FOXP3+ regulatory T cells use heparanase to access IL-2 bound to ECM in inflamed tissues
Hunter A. Martinez, Ievgen Koliesnik, Gernot Kaber, Jacqueline K. Reid, Nadine Nagy, Graham Barlow, Ben A. Falk, Carlos O. Medina, Aviv Hargil, Israel Vlodavsky, Jin-Ping Li, Magdiel Pérez-Cruz, Sai-Wen Tang, Everett H. Meyer, Lucile E. Wrenshall, James D. Lord, K. Christopher Garcia, Theo D. Palmer, Lawrence Steinman, Gerald T. Nepom, Thomas N. Wight, Paul L. Bollyky, Hedwich F. Kuipers
bioRxiv 2023.02.26.529772; doi: https://doi.org/10.1101/2023.02.26.529772

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