Desferrioxamine Treatment Prevents Chronic Islet Allograft Damage

Author:

Bradley Brenda1,Prowse Stephen J1,Bauling Paul1,Lafferty Kevin J1

Affiliation:

1. Barbara Davis Center for Childhood Diabetes, Departments of Microbiology and Immunology, Pediatrics and Surgery, the University of Colorado Health Sciences Center Denver, Colorado 80262

Abstract

BALB/cByJ islet allografts are acutely rejected when transplanted into allogeneic mice (CBA/J). Culture of the tissue for 7 days in 95% O2 before grafting is a suboptimal treatment for the reduction of immunogenicity in this strain combination. Approximately half the animals reject these transplants in a chronic fashion. Chronic islet rejection differs from acute rejection of uncultured allogeneic islets. During chronic rejection, beta cells within the transplanted tissue degranulate but remain intact when the animal returns to the diabetic condition. Acute islet rejection is characterized by the destruction of beta cells that remain heavily granulated as long as they remain intact. We examined the effect of the iron chelating agent, desferrioxamine, on chronic islet allograft damage. Desferrioxamine inhibited chronic islet allograft damage but did not influence the process of rejection of uncultured islet tissue. This effect of desferrioxamine could not be attributed to a direct immunosuppressive effect of this agent.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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1. The role of ferroptosis in metabolic diseases;Biochimica et Biophysica Acta (BBA) - Molecular Cell Research;2023-08

2. Bilirubin Protects Transplanted Islets by Targeting Ferroptosis;Frontiers in Pharmacology;2020-06-16

3. Pancreas and islet preservation;Transplantation, Bioengineering, and Regeneration of the Endocrine Pancreas;2020

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5. Regulated Cell Death Seen through the Lens of Islet Transplantation;Cell Transplantation;2018-05-30

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