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Structural insertion/deletion variation in IRF5 is associated with a risk haplotype and defines the precise IRF5 isoforms expressed in systemic lupus erythematosus

✍ Scribed by Sergey V. Kozyrev; Susanna Lewén; Prasad M. V. Linga Reddy; Bernardo Pons-Estel; Argentine Collaborative Group; Torsten Witte; German Collaborative Group; Peter Junker; Helle Laustrup; Carmen Gutiérrez; Ana Suárez; Maria Francisca González-Escribano; Javier Martín; Spanish Collaborative Group; Marta E. Alarcón-Riquelme

Publisher
John Wiley and Sons
Year
2007
Tongue
English
Weight
234 KB
Volume
56
Category
Article
ISSN
0004-3591

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✦ Synopsis

Abstract

Objective

To determine whether specific isoforms of IRF5 are transcribed in patients with systemic lupus erythematosus (SLE) who have risk genotypes in the exon 1B donor splice site at single‐nucleotide polymorphism (SNP) no. rs2004640.

Methods

Peripheral blood mononuclear cells were obtained from SLE patients and healthy controls from Argentina, Spain, and Germany and from trio families from Spain and Denmark. A reporter assay was used to investigate the role of SNP no. rs2004640. IRF5 expression in relation to the genotypes of functional SNPs was analyzed using quantitative polymerase chain reaction. Sequencing and genotyping of the IRF5 gene was performed.

Results

Sequencing of complementary DNA from individuals with different genotypes showed 4 basic isoforms transcribed from all 5′‐untranslated regions (5′‐UTRs), suggesting no preferential isoform transcription based on rs2004640 genotypes. Analysis of translation efficiency showed that exon 1A was the most efficient in initiating protein synthesis. We identified a novel polymorphic insertion/deletion that defines the pattern of expression of isoforms of IRF5. The insertion consists of 4 repeats in exon 6 affecting the protein interaction domain. The insertion segregates in the risk haplotype with the high expression allele of a poly(A) site SNP no. rs10954213 and the exon 1B donor splice allele of the 5′‐UTR SNP no. rs2004640. The poly(A) polymorphism correlated with levels of IRF5 in cells stimulated with interferon‐α. The SNP most strongly associated with SLE was SNP no. rs2070197 (P = 5.2 × 10^−11^), which is a proxy of the risk haplotype, but does not appear to be functional.

Conclusion

None of the functional variants investigated in this study is strongly associated with SLE, with the exception of the exon 1B donor splice site, and its functional importance appears to be small. Our results suggest that there may be other functional polymorphisms, yet to be identified, in IRF5. We did not observe evidence of epistatic interaction between the functional SNPs.

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