Donor bone marrow cells are essential for iNKT cell-mediated Foxp3+ Treg cell expansion in a murine model of transplantation tolerance
Author:
Affiliation:
1. Department of Urology; Tokyo Women's Medical University; Tokyo Japan
2. Department of Cardiovascular Surgery; Tokyo Women's Medical University; Tokyo Japan
3. Cluster for Industry Partnerships (CIP); RIKEN; Yokohama Kanagawa Japan
Funder
Japanese Urological Association
Publisher
Wiley
Subject
Immunology,Immunology and Allergy
Reference48 articles.
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2. Mixed chimerism: preclinical studies and clinical applications;McSweeney;Biol. Blood Marrow Transplant,1999
3. Immune tolerance: mechanisms and application in clinical transplantation;Sykes;J. Intern. Med.,2007
4. Prevention of acute and chronic allograft rejection with CD4+CD25+Foxp3+ regulatory T lymphocytes;Joffre;Nat. Med.,2008
5. Treg-therapy allows mixed chimerism and transplantation tolerance without cytoreductive conditioning;Pilat;Am. J. Transplant,2010
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3. Expansion and CD2/CD3/CD28 stimulation enhance Th2 cytokine secretion of human invariant NKT cells with retained anti-tumor cytotoxicity;Cytotherapy;2020-05
4. Combination therapy of an iNKT cell ligand and CD40–CD154 blockade establishes islet allograft acceptance in nonmyeloablative bone marrow transplant recipients;Acta Diabetologica;2019-02-13
5. The Role of Invariant NKT in Autoimmune Liver Disease: Can Vitamin D Act as an Immunomodulator?;Canadian Journal of Gastroenterology and Hepatology;2018-06-26
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