The effect of type 1 diabetes protection and susceptibility associated HLA class II genotypes on DNA methylation in immune cells

dc.contributor.authorPahkuri, Sirpa
dc.contributor.authorKatayama, Shintaro
dc.contributor.authorValta, Milla
dc.contributor.authorNygård, Lucas
dc.contributor.authorKnip, Mikael
dc.contributor.authorKere, Juha
dc.contributor.authorIlonen, Jorma
dc.contributor.authorLempainen, Johanna
dc.contributor.authorFinnish Pediatric Diabetes Register
dc.contributor.organizationfi=biolääketieteen laitos|en=Institute of Biomedicine|
dc.contributor.organizationfi=tyks, vsshp|en=tyks, varha|
dc.contributor.organization-code1.2.246.10.2458963.20.77952289591
dc.contributor.organization-code2607100
dc.converis.publication-id456989571
dc.converis.urlhttps://research.utu.fi/converis/portal/Publication/456989571
dc.date.accessioned2025-08-27T21:45:11Z
dc.date.available2025-08-27T21:45:11Z
dc.description.abstractThe HLA region, especially HLA class I and II genes, which encode molecules for antigen presentation to T cells, plays a major role in the predisposition to autoimmune disorders. To clarify the mechanisms behind this association, we examined genome-wide DNA methylation by microarrays to cover over 850,000 CpG sites in the CD4<sup>+</sup> T cells and CD19<sup>+</sup> B cells of healthy subjects homozygous either for DRB1*15-DQA1*01-DQB1*06:02 (DR2-DQ6, n = 14), associated with a strongly decreased T1D risk, DRB1*03-DQA1*05-DQB1*02 (DR3-DQ2, n = 19), or DRB1*04:01-DQA1*03-DQB1*03:02 (DR4-DQ8, n = 17), associated with a moderately increased T1D risk. In total, we discovered 14 differentially methylated CpG probes, of which 10 were located in the HLA region and six in the HLA-DRB1 locus. The main differences were between the protective genotype DR2-DQ6 and the risk genotypes DR3-DQ2 and DR4-DQ8, where the DR2-DQ6 group was hypomethylated compared to the other groups in all but four of the differentially methylated probes. The differences between the risk genotypes DR3-DQ2 and DR4-DQ8 were small. Our results indicate that HLA variants have few systemic effects on methylation and that their effect on autoimmunity is conveyed directly by HLA molecules, possibly by differences in expression levels or function.
dc.identifier.eissn2059-2310
dc.identifier.jour-issn2059-2302
dc.identifier.olddbid201039
dc.identifier.oldhandle10024/184066
dc.identifier.urihttps://www.utupub.fi/handle/11111/47437
dc.identifier.urlhttps://doi.org/10.1111/tan.15548
dc.identifier.urnURN:NBN:fi-fe2025082789307
dc.language.isoen
dc.okm.affiliatedauthorPahkuri, Sirpa
dc.okm.affiliatedauthorValta, Milla
dc.okm.affiliatedauthorNygård, Lucas
dc.okm.affiliatedauthorIlonen, Jorma
dc.okm.affiliatedauthorLempainen, Johanna
dc.okm.affiliatedauthorDataimport, tyks, vsshp
dc.okm.discipline3111 Biomedicineen_GB
dc.okm.internationalcopublicationinternational co-publication
dc.okm.internationalityInternational publication
dc.okm.typeA1 ScientificArticle
dc.publisherWiley-Blackwell
dc.publisher.countryUnited Kingdomen_GB
dc.publisher.countryBritanniafi_FI
dc.publisher.country-codeGB
dc.relation.articlenumbere15548
dc.relation.doi10.1111/tan.15548
dc.relation.ispartofjournalHLA
dc.relation.issue6
dc.relation.volume103
dc.source.identifierhttps://www.utupub.fi/handle/10024/184066
dc.titleThe effect of type 1 diabetes protection and susceptibility associated HLA class II genotypes on DNA methylation in immune cells
dc.year.issued2024

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