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IFN-α induces a preferential long-lasting expression of MHC class I in human pancreatic beta cells.

Citation
de Brachène, A. C., et al. “Ifn-Α Induces A Preferential Long-Lasting Expression Of Mhc Class I In Human Pancreatic Beta Cells.”. Diabetologia, pp. 636-640.
Center Indiana University
Author Alexandra Coomans de Brachène, Reinaldo S Dos Santos, Laura Marroqui, Maikel L Colli, Lorella Marselli, Raghavendra G Mirmira, Piero Marchetti, Decio L Eizirik
Keywords IFN-α, JAK inhibitors, MHC class I, pancreatic beta cells, pancreatic islets, type 1 diabetes
Abstract

AIMS/HYPOTHESIS: IFN-α, a cytokine expressed in human islets from individuals affected by type 1 diabetes, plays a key role in the pathogenesis of diabetes by upregulating inflammation, endoplasmic reticulum (ER) stress and MHC class I overexpression, three hallmarks of islet histology in early type 1 diabetes. We tested whether expression of these mediators of beta cell loss is reversible upon IFN-α withdrawal or IFN-α pathway inhibition.

METHODS: IFN-α-induced MHC class I overexpression, ER stress and inflammation were evaluated by flow cytometry, immunofluorescence and real-time PCR in human EndoC-βH1 cells or human islets exposed to IFN-α with or without the presence of Janus kinase (JAK) inhibitors. Protein expression was evaluated by western blot.

RESULTS: IFN-α-induced expression of inflammatory and ER stress markers returned to baseline after 24-48 h following cytokine removal. In contrast, MHC class I overexpression at the cell surface persisted for at least 7 days. Treatment with JAK inhibitors, when added with IFN-α, prevented MHC class I overexpression, but when added 24 h after IFN-α exposure these inhibitors failed to accelerate MHC class I return to baseline.

CONCLUSIONS/INTERPRETATION: IFN-α mediates a long-lasting and preferential MHC class I overexpression in human beta cells, which is not affected by the subsequent addition of JAK inhibitors. These observations suggest that IFN-α-stimulated long-lasting MHC class I expression may amplify beta cell antigen presentation during the early phase of type 1 diabetes and that IFN-α inhibitors might need to be used at very early stages of the disease to be effective.

Year of Publication
2018
Journal
Diabetologia
Volume
61
Issue
3
Number of Pages
636-640
Date Published
12/2018
ISSN Number
1432-0428
DOI
10.1007/s00125-017-4536-4
Alternate Journal
Diabetologia
PMID
29305625
PMCID
PMC6241216
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