4.8 Article

Support for involvement of neuregulin 1 in schizophrenia pathophysiology

Journal

MOLECULAR PSYCHIATRY
Volume 10, Issue 4, Pages 366-374

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/sj.mp.4001608

Keywords

linkage disequilibrium; haplotypes; oligonucleotide array sequence analysis; gene expression; single nucleotide-polymorphisms; transcript variant

Funding

  1. NIMH NIH HHS [MH 52618, MH 058693] Funding Source: Medline

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Schizophrenia is a common, multigenic psychiatric disorder. Linkage studies, including a recent meta-analysis of genome scans, have repeatedly implicated chromosome 8p12-p23.1 in schizophrenia susceptibility. More recently, significant association with a candidate gene on 8p12, neuregulin 1 (NRG1), has been reported in several European and Chinese samples. We investigated NRG1 for association in schizophrenia patients of Portuguese descent to determine whether this gene is a risk factor in this population. We tested NRG1 markers and haplotypes for association in 111 parent-proband trios, 321 unrelated cases, and 242 control individuals. Associations were found with a haplotype that overlaps the risk haplotype originally reported in the Icelandic population ('Hap(ICE)'), and two haplotypes located in the 30 end of NRG1 ( all P<0.05). However, association was not detected with Hap(ICE) itself. Comparison of NRG1 transcript expression in peripheral leukocytes from schizophrenia patients and unaffected siblings identified 3.8-fold higher levels of the SMDF variant in patients ( P = 0.039). Significant positive correlations ( P<0.001) were found between SMDF and HRG-beta 2 expression and between HRG-gamma and ndf43 expression, suggesting common transcriptional regulation of NRG1 variants. In summary, our results suggest that haplotypes across NRG1 and multiple NRG1 variants are involved in schizophrenia.

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