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dc.contributor.authorKrogvold, L
dc.contributor.authorLeete, P
dc.contributor.authorMynarek, IM
dc.contributor.authorRussell, MA
dc.contributor.authorGerling, IC
dc.contributor.authorLenchik, NI
dc.contributor.authorMathews, C
dc.contributor.authorRichardson, SJ
dc.contributor.authorMorgan, NG
dc.contributor.authorDahl-Jørgensen, K
dc.date.accessioned2022-07-27T09:50:01Z
dc.date.issued2022-07-26
dc.date.updated2022-07-27T08:35:23Z
dc.description.abstractAims/hypothesis: The Diabetes Virus Detection (DiViD) study has suggested the presence of low-grade enteroviral infection in pancreatic tissue collected from six of six live adult patients newly diagnosed with type 1 diabetes. The present study aimed to compare the gene and protein expression of selected virally induced pathogen recognition receptors and interferon stimulated genes in islets from these newly diagnosed type 1 diabetes (DiViD) subjects vs age-matched non-diabetic (ND) controls. Methods: RNA was extracted from laser-captured islets and Affymetrix Human Gene 2.0 ST arrays used to obtain gene expression profiles. Lists of differentially expressed genes were subjected to a data-mining pipeline searching for enrichment of canonical pathways, KEGG pathways, Gene Ontologies, transcription factor binding sites and other upstream regulators. In addition, the presence and localisation of specific viral response proteins (PKR, MxA and MDA5) were examined by combined immunofluorescent labelling in sections of pancreatic tissue. Results: The data analysis and data mining process revealed a significant enrichment of gene ontologies covering viral reproduction and infectious cycles; peptide translation, elongation and initiation, as well as oxidoreductase activity. Enrichment was identified in the KEGG pathways for oxidative phosphorylation; ribosomal and metabolic activity; antigen processing and presentation and in canonical pathways for mitochondrial dysfunction, oxidative phosphorylation and EIF2 signaling. Protein Kinase R (PKR) expression did not differ between newly diagnosed type 1 diabetes and ND islets at the level of total RNA, but a small subset of b-cells displayed markedly increased PKR protein levels. These PKR+ b-cells correspond to those previously shown to contain the viral protein, VP1. RNA encoding MDA5 was increased significantly in newly diagnosed type 1 diabetes islets, and immunostaining of MDA5 protein was seen in a- and certain b-cells in both newly diagnosed type 1 diabetes and ND islets, but the expression was increased in b-cells in type 1 diabetes. In addition, an uncharacterised subset of synaptophysin positive, but islet hormone negative, cells expressed intense MDA5 staining and these were more prevalent in DiViD cases. MxA RNA was upregulated in newly diagnosed type 1 diabetes vs ND islets and MxA protein was detected exclusively in newly diagnosed type 1 diabetes b-cells. Conclusion/interpretation: The gene expression signatures reveal that pathways associated with cellular stress and increased immunological activity are enhanced in islets from newly diagnosed type 1 diabetes patients compared to controls. The increases in viral response proteins seen in b-cells in newly diagnosed type 1 diabetes provide clear evidence for the activation of IFN signalling pathways. As such, these data strengthen the hypothesis that an enteroviral infection of islet b-cells contributes to the pathogenesis of type 1 diabetes.en_GB
dc.description.sponsorshipEuropean Unionen_GB
dc.description.sponsorshipJuvenile Diabetes Research Foundation Internationalen_GB
dc.description.sponsorshipJuvenile Diabetes Research Foundation Internationalen_GB
dc.description.sponsorshipMedical Research Councilen_GB
dc.description.sponsorshipNational Institute for Health Researchen_GB
dc.description.sponsorshipJuvenile Diabetes Research Foundationen_GB
dc.description.sponsorshipJuvenile Diabetes Research Foundationen_GB
dc.description.sponsorshipLeona M & Harry B Helmsley Charitable Trusten_GB
dc.description.sponsorshipSouth-Eastern Norway Regional Health Authorityen_GB
dc.description.sponsorshipNovo Nordisk Foundationen_GB
dc.identifier.citationVol. 13, article 881997en_GB
dc.identifier.doihttps://doi.org/10.3389/fendo.2022.881997
dc.identifier.grantnumberFP7/2007-2013en_GB
dc.identifier.grantnumber5-CDA-2014-221-A-Nen_GB
dc.identifier.grantnumberJDRF 25-2012-516en_GB
dc.identifier.grantnumberMR/P010695/1en_GB
dc.identifier.grantnumberDK104155en_GB
dc.identifier.grantnumberJDRF 25-2010-723en_GB
dc.identifier.grantnumberJDRF 47-2013-520en_GB
dc.identifier.grantnumber2018PG-type 1 diabetes053en_GB
dc.identifier.urihttp://hdl.handle.net/10871/130414
dc.identifierORCID: 0000-0002-1160-6062 (Richardson, Sarah J)
dc.identifierScopusID: 24601185100 (Richardson, Sarah J)
dc.language.isoenen_GB
dc.publisherFrontiers Mediaen_GB
dc.rightsCopyright © 2022 Krogvold, Leete, Mynarek, Russell, Gerling, Lenchik, Mathews, Richardson, Morgan and Dahl-Jørgensen. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.en_GB
dc.subjectbiopsyen_GB
dc.subjectenterovirusen_GB
dc.subjectgene expressionen_GB
dc.subjectMDA5en_GB
dc.subjectMxAen_GB
dc.subjectpancreasen_GB
dc.subjectPKRen_GB
dc.subjectType 1 diabetesen_GB
dc.titleDetection of antiviral tissue responses and increased cell stress in the pancreatic islets of newly diagnosed Type 1 diabetes patients: results from the DiViD studyen_GB
dc.typeArticleen_GB
dc.date.available2022-07-27T09:50:01Z
dc.descriptionThis is the final version. Available from Frontiers Media via the DOI in this record.en_GB
dc.descriptionDATA AVAILABILITY STATEMENT: The datasets presented in this article are not readily available because of the sensitive nature of the data and possible high risks associated with patient confidentiality. Requests to access the datasets should be directed to the authors.en_GB
dc.identifier.eissn1664-2392
dc.identifier.journalFrontiers in Endocrinologyen_GB
dc.relation.ispartofFrontiers in Endocrinology, 13
dc.rights.urihttps://creativecommons.org/licenses/by/4.0/en_GB
dcterms.dateAccepted2022-05-27
rioxxterms.versionVoRen_GB
rioxxterms.licenseref.startdate2022-07-26
rioxxterms.typeJournal Article/Reviewen_GB
refterms.dateFCD2022-07-27T09:42:57Z
refterms.versionFCDVoR
refterms.dateFOA2022-07-27T09:50:02Z
refterms.panelAen_GB
refterms.dateFirstOnline2022-07-26


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Copyright © 2022 Krogvold, Leete, Mynarek, Russell, Gerling, Lenchik, Mathews,
Richardson, Morgan and Dahl-Jørgensen. This is an open-access article distributed
under the terms of the Creative Commons Attribution License (CC BY). The use,
distribution or reproduction in other forums is permitted, provided the original
author(s) and the copyright owner(s) are credited and that the original publication in
this journal is cited, in accordance with accepted academic practice. No use,
distribution or reproduction is permitted which does not comply with these terms.
Except where otherwise noted, this item's licence is described as Copyright © 2022 Krogvold, Leete, Mynarek, Russell, Gerling, Lenchik, Mathews, Richardson, Morgan and Dahl-Jørgensen. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.