Fine-mapping resolves Eae23 into two QTLs and implicates ZEB1 as a candidate gene regulating experimental neuroinflammation in rat

Pernilla Stridh; Melanie Thessen Hedreul; Amennai Daniel Beyeen; Milena Z Adzemovic; Hannes Laaksonen; Alan Gillett; Johan Ockinger; Monica Marta; Hans Lassmann; Kristina Becanovic; Maja Jagodic; Tomas Olsson

doi:10.1371/journal.pone.0012716

Fine-mapping resolves Eae23 into two QTLs and implicates ZEB1 as a candidate gene regulating experimental neuroinflammation in rat

PLoS One. 2010 Sep 15;5(9):e12716. doi: 10.1371/journal.pone.0012716.

Authors

Pernilla Stridh¹, Melanie Thessen Hedreul, Amennai Daniel Beyeen, Milena Z Adzemovic, Hannes Laaksonen, Alan Gillett, Johan Ockinger, Monica Marta, Hans Lassmann, Kristina Becanovic, Maja Jagodic, Tomas Olsson

Affiliation

¹ Center for Molecular Medicine, Department of Clinical Neuroscience, Neuroimmunology Unit, Karolinska Institutet, Stockholm, Sweden. pernilla.strid@ki.se

Abstract

Background: To elucidate mechanisms involved in multiple sclerosis (MS), we studied genetic regulation of experimental autoimmune encephalomyelitis (EAE) in rats, assuming a conservation of pathogenic pathways. In this study, we focused on Eae23, originally identified to regulate EAE in a (LEW.1AV1xPVG.1AV1)F2 cross. Our aim was to determine whether one or more genes within the 67 Mb region regulate EAE and to define candidate risk genes.

Methodology/principal findings: We used high resolution quantitative trait loci (QTL) analysis in the 10th generation (G10) of an advanced intercross line (AIL) to resolve Eae23 into two QTLs that independently regulate EAE, namely Eae23a and Eae23b. We established a congenic strain to validate the effect of this region on disease. PVG alleles in Eae23 resulted in significant protection from EAE and attenuated CNS inflammation/demyelination. Disease amelioration was accompanied with increased levels of Foxp3(+) cells in the CNS of the congenic strain compared to DA. We then focused on candidate gene investigation in Eae23b, a 9 Mb region linked to all clinical phenotypes. Affymetrix exon arrays were used to study expression of the genes in Eae23b in the parental strains, where none showed differential expression. However, we found lower expression of exon 4 of ZEB1, which is specific for splice-variant Zfhep1. ZEB1 is an interleukin 2 (IL2) repressor involved in T cell development. The splice-specific variance prompted us to next analyze the expression of ZEB1 and its two splice variants, Zfhep1 and Zfhep2, in both lymph node and spleen. We demonstrated that ZEB1 splice-variants are differentially expressed; severity of EAE and higher IL2 levels were associated with down-regulation of Zfhep1 and up-regulation of Zfhep2.

Conclusions/significance: We speculate that the balance between splice-variants of ZEB1 could influence the regulation of EAE. Further functional studies of ZEB1 and the splice-variants may unravel novel pathways contributing to MS pathogenesis and inflammation in general.

Publication types

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

MeSH terms

Animals
Chromosome Mapping
Encephalomyelitis, Autoimmune, Experimental / genetics*
Encephalomyelitis, Autoimmune, Experimental / immunology
Female
Gene Expression Regulation
Homeodomain Proteins / genetics*
Homeodomain Proteins / immunology
Humans
Male
Multiple Sclerosis / genetics*
Multiple Sclerosis / immunology
Quantitative Trait Loci*
RNA Splicing
Rats
Transcription Factors / genetics*
Transcription Factors / immunology
Zinc Finger E-box-Binding Homeobox 1

Substances

Homeodomain Proteins
Transcription Factors
ZEB1 protein, rat
Zinc Finger E-box-Binding Homeobox 1