Autoantibody and T cell responses to oxidative post-translationally modified insulin neoantigenic peptides in type 1 diabetes

Rocky Strollo; Chiara Vinci; Y K Stella Man; Sara Bruzzaniti; Erica Piemonte; Ghadeer Alhamar; Silvia Irina Briganti; Ilaria Malandrucco; Flavia Tramontana; Chiara Fanali; James Garnett; Roberto Buccafusca; Perrin Guyer; Mark Mamula; Eddie A James; Paolo Pozzilli; Johnny Ludvigsson; Paul G Winyard; Mario Galgani; Ahuva Nissim

doi:10.1007/s00125-022-05812-4

Autoantibody and T cell responses to oxidative post-translationally modified insulin neoantigenic peptides in type 1 diabetes

Diabetologia. 2023 Jan;66(1):132-146. doi: 10.1007/s00125-022-05812-4. Epub 2022 Oct 7.

Authors

Rocky Strollo¹, Chiara Vinci², Y K Stella Man², Sara Bruzzaniti^{3

4}, Erica Piemonte⁵, Ghadeer Alhamar⁶, Silvia Irina Briganti⁶, Ilaria Malandrucco⁷, Flavia Tramontana⁶, Chiara Fanali¹, James Garnett^{8

9}, Roberto Buccafusca⁹, Perrin Guyer¹⁰, Mark Mamula¹¹, Eddie A James¹⁰, Paolo Pozzilli⁶, Johnny Ludvigsson¹², Paul G Winyard¹³, Mario Galgani^{3

5}, Ahuva Nissim¹⁴

Affiliations

¹ Department of Science and Technology for Humans and the Environment, Università Campus Bio-Medico di Roma, Rome, Italy.
² Biochemical Pharmacology, William Harvey Research Institute, Queen Mary University of London, London, UK.
³ Institute for Experimental Endocrinology and Oncology 'G. Salvatore', Consiglio Nazionale delle Ricerche, Naples, Italy.
⁴ Department of Biology, Università degli Studi di Napoli 'Federico II', Naples, Italy.
⁵ Department of Molecular Medicine and Medical Biotechnology, Università degli Studi di Napoli 'Federico II', Naples, Italy.
⁶ Department of Medicine, Unit of Endocrinology & Diabetes, Università Campus Bio-Medico di Roma, Rome, Italy.
⁷ The UOSD of Endocrinology and Metabolic Diseases, Azienda Sanitaria Locale (ASL) Frosinone, Frosinone, Italy.
⁸ Centre for Host-Microbiome Interactions, Dental Institute, King's College London, London, UK.
⁹ School of Biological and Chemical Sciences, Queen Mary University of London, London, UK.
¹⁰ Program for Translational Immunology, Benaroya Research Institute, Seattle, WA, USA.
¹¹ Department of Medicine, Yale University School of Medicine, New Haven, CT, USA.
¹² Division of Pediatrics, Department of Biomedical and Clinical Sciences, Crown Princess Victoria Children's Hospital, Linköping University, Linköping, Sweden.
¹³ Institute of Biomedical and Clinical Science, University of Exeter Medical School, St Luke's Campus, Exeter, UK.
¹⁴ Biochemical Pharmacology, William Harvey Research Institute, Queen Mary University of London, London, UK. a.nissim@qmul.ac.uk.

Abstract

Aims/hypothesis: Antibodies specific to oxidative post-translational modifications (oxPTM) of insulin (oxPTM-INS) are present in most individuals with type 1 diabetes, even before the clinical onset. However, the antigenic determinants of such response are still unknown. In this study, we investigated the antibody response to oxPTM-INS neoepitope peptides (oxPTM-INSPs) and evaluated their ability to stimulate humoral and T cell responses in type 1 diabetes. We also assessed the concordance between antibody and T cell responses to the oxPTM-INS neoantigenic peptides.

Methods: oxPTM-INS was generated by exposing insulin to various reactive oxidants. The insulin fragments resulting from oxPTM were fractionated by size-exclusion chromatography further to ELISA and LC-MS/MS analysis to identify the oxidised peptide neoepitopes. Immunogenic peptide candidates were produced and then modified in house or designed to incorporate in silico-oxidised amino acids during synthesis. Autoantibodies to the oxPTM-INSPs were tested by ELISA using sera from 63 participants with new-onset type 1 diabetes and 30 control participants. An additional 18 fresh blood samples from participants with recently diagnosed type 1 diabetes, five with established disease, and from 11 control participants were used to evaluate, in parallel, CD4⁺ and CD8⁺ T cell activation by oxPTM-INSPs.

Results: We observed antibody and T cell responses to three out of six LC-MS/MS-identified insulin peptide candidates: A:12-21 (SLYQLENYCN, native insulin peptide 3 [Nt-INSP-3]), B:11-30 (LVEALYLVCGERGFFYTPKT, Nt-INSP-4) and B:21-30 (ERGFFYTPKT, Nt-INSP-6). For Nt-INSP-4 and Nt-INSP-6, serum antibody binding was stronger in type 1 diabetes compared with healthy control participants (p≤0.02), with oxidised forms of ERGFFYTPKT, oxPTM-INSP-6 conferring the highest antibody binding (83% binders to peptide modified in house by hydroxyl radical [^●OH] and >88% to in silico-oxidised peptide; p≤0.001 vs control participants). Nt-INSP-4 induced the strongest T cell stimulation in type 1 diabetes compared with control participants for both CD4⁺ (p<0.001) and CD8⁺ (p=0.049). CD4⁺ response to oxPTM-INSP-6 was also commoner in type 1 diabetes than in control participants (66.7% vs 27.3%; p=0.039). Among individuals with type 1 diabetes, the CD4⁺ response to oxPTM-INSP-6 was more frequent than to Nt-INSP-6 (66.7% vs 27.8%; p=0.045). Overall, 44.4% of patients showed a concordant autoimmune response to oxPTM-INSP involving simultaneously CD4⁺ and CD8⁺ T cells and autoantibodies.

Conclusions/interpretation: Our findings support the concept that oxidative stress, and neoantigenic epitopes of insulin, may be involved in the immunopathogenesis of type 1 diabetes.

Keywords: Autoimmunity; Immune response; Insulin; Insulin autoantibodies; Insulin neoepitope peptide; Neoantigen; Neoepitope; Oxidative post-translational modifications; Post-translational modifications.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Autoantibodies
CD8-Positive T-Lymphocytes
Chromatography, Liquid
Diabetes Mellitus, Type 1*
Humans
Insulin*
Tandem Mass Spectrometry

Substances

Insulin
Autoantibodies

Grants and funding

UL1 TR001863/TR/NCATS NIH HHS/United States