Residual methylprednisolone suppresses human T-cell responses to spleen, but not islet, extracts from deceased organ donors

Pancreatic islets, transplanted into recipients with type 1 diabetes, are exposed to allogenic and auto-immune T-cell responses. We set out to develop an assay to measure these responses using PBMC. Our approach was to prepare spleen extract from the islet donors (allo-antigen) and islet extracts (a...

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Bibliographic Details
Published in:International immunology 2012-07, Vol.24 (7), p.447-453
Main Authors: Joffe, Max, Necula, Andra S, Chand, Rochna, McWhinney, Brett C, Krishnamurthy, Balasubramanian, Loudovaris, Tom, Goodman, David, Thomas, Helen E, Kay, Thomas W H, Mannering, Stuart I
Format: Article
Language:English
Subjects:
Autoantigens
Autoantigens - immunology
CD152 antigen
Cell Extracts - chemistry
Cell Extracts - immunology
Cell Extracts - pharmacology
Cell proliferation
Cell Proliferation - drug effects
Cells, Cultured
CTLA-4 protein
Diabetes mellitus
Diabetes Mellitus, Type 1 - immunology
Diabetes Mellitus, Type 1 - therapy
Donors
Glucocorticoid receptors
Glucocorticoids
Hot Temperature
Humans
Immunosuppression
Islets of Langerhans
Islets of Langerhans - chemistry
Islets of Langerhans - immunology
Islets of Langerhans Transplantation - immunology
Isoantigens - immunology
Lymphocyte Activation - drug effects
Lymphocytes T
Mass Spectrometry
Mass spectroscopy
methylprednisolone
Methylprednisolone - analysis
Methylprednisolone - pharmacology
mifepristone
Mifepristone - pharmacology
Mitogens
Monoclonal antibodies
Pancreas
Pancreas transplantation
Pancreatic islet transplantation
Peripheral blood mononuclear cells
Proteinase
Reducing agents
Spleen
Spleen - chemistry
Spleen - immunology
T-Lymphocytes - drug effects
T-Lymphocytes - immunology
Tetanus
Tissue Donors
Transforming growth factor- beta
Vaccines
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Summary:Pancreatic islets, transplanted into recipients with type 1 diabetes, are exposed to allogenic and auto-immune T-cell responses. We set out to develop an assay to measure these responses using PBMC. Our approach was to prepare spleen extract from the islet donors (allo-antigen) and islet extracts (auto-antigen). To our surprise, we found that spleen extracts potently inhibited the proliferation of human T cells driven by antigen (tetanus toxoid) and mitogen (anti-CD3 mAb, OKT3), whereas extracts prepared from pancreatic islets from the same donor did not suppress T-cell proliferation. Suppression mediated by spleen extracts was unaffected by blocking mAbs against the IL-10R, transforming growth factor-β or CD152 (CTLA-4). It was also unaffected by denaturing the spleen extracts by heating, exposing to reducing agents or protease digestion. Because deceased organ donors are commonly given the immunosuppressive glucocorticoid methylprednisolone prior to death, we hypothesized that suppression was due to residual methylprednisolone in the spleen extracts. Methylprednisolone could be detected by mass spectrometry in spleen extracts at concentrations that suppress T-cell proliferation. Finally, the glucocorticoid receptor antagonist mifepristone completely reversed the suppression caused by the spleen extracts. We conclude that extracts of human spleen, but not islets, from deceased organ donors contain sufficient residual methylprednisolone to suppress the proliferation of T-cells in vitro.
ISSN:0953-8178
1460-2377
DOI:10.1093/intimm/dxs042