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Association of HLA class I markers with multiple sclerosis in the Italian and UK population: Evidence of two independent protective effects

  • Laura Bergamaschi
  • , Maria Ban
  • , Nadia Barizzone
  • , Maurizio Leone
  • , Daniela Ferrante
  • , Maria Edvige Fasano
  • , Franca R. Guerini
  • , Lucia Corrado
  • , Paola Naldi
  • , Ennia Dametto
  • , Cristina Agliardi
  • , Marco Salvetti
  • , Rosella Mechelli
  • , Daniela Galimberti
  • , Elio Scarpini
  • , Paola Cavalla
  • , Valeria Bargiggia
  • , Domenico Caputo
  • , Susanna Cordera
  • , Francesco Monaco
  • Patricia Momigliano-Richiardi, Sandra D'Alfonso

Research output: Contribution to journalArticlepeer-review

Abstract

Background The association of HLA A*02 with multiple sclerosis (MS) was recently confirmed by the authors, and it was observed that the combined presence of HLA Cw*05 significantly enhanced (threefold) the protective effect of HLA A*02. Objectives and methods Since A*02-Cw*05 is carried by two HLA extended haplotypes characterised by the B*4402 and B*1801 alleles, respectively, the association analysis was extended to HLA B*44 and B*18 in an Italian sample (1445 MS cases and 973 controls) and these associations were verified in a UK cohort (721 MS cases, 408 controls and 480 family trios). Results A strong protective effect, independent of DR15, of the A*02-Cw*05 combination carrying B*44 (OR 0.27, p=3.3×10-5) was seen in the Italian samples and confirmed in UK family trios (OR 0.33, p=5.5×10-4) and in a combined cohort of UK families and caseecontrols (OR 0.53, p=0.044). This protective effect was significantly stronger than that mediated by A*02 alone. Logistic regression showed that A*02-Cw*05 maintained a significant protection when adjusted for B alleles (Italy: OR 0.38, p=6.5×10-7; UK: OR 0.60, p=0.0029), indicating that it was not secondary to linkage disequilibrium with B*44. Different from A*02, the other HLA class I tested markers individually showed no significant (Cw*05, B*18) or a modest (B*44) protection when adjusted for the remaining markers. Conclusions This study identified at least two independent protective effects which are tagged by A*02eCw*05 and A*02, respectively. Further studies are needed to elucidate whether this protective effect is due to the presence of an unanalysed factor characterising the HLA extended haplotype(s) carrying A*02 and Cw*05 or to a direct interaction between these alleles.

Original languageEnglish
Pages (from-to)485-492
Number of pages8
JournalJournal of Medical Genetics
Volume48
Issue number7
DOIs
Publication statusPublished - Jul 2011

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