Nogo receptor 1 (RTN4R) as a candidate gene for schizophrenia: Analysis using human and mouse genetic approaches

Authors

Ruby Hsu, Columbia University
Abigail Woodroffe, University of Michigan, Ann Arbor
Wen Sung Lai, Vagelos College of Physicians and Surgeons
Melloni N. Cook, University of Memphis
Jun Mukai, Vagelos College of Physicians and Surgeons
Jonathan P. Dunning, University of Memphis
Douglas J. Swanson, University of Tennessee Health Science Center
J. Louw Roos, University of Pretoria

Abstract

Background. NOGO Receptor 1 (RTN4R) regulates axonal growth, as well as axort regeneration after injury. The gene maps to the 22q11.2 schizophrenia susceptibility locus and is thus a strong functional and positional candidate gene. Methodology/Principal Findings. We evaluate evidence for genetic association between common RTN4R polymorphisms and schizophrenia in a large family sample of Afrikaner origin and screen the exonic sequence of RTN4R for rare variants in an independent sample from the U.S. We also employ animal model studies to assay a panel of schizophrenia-related behavioral tasks in an Rtn4r-deficient mouse model. We found weak sex-specific evidence for association between common RTN4R polymorphisms and schizophrenia in the Afrikaner patients. In the U.S. sample, we identified two novel non-conservative RTN4R coding variants in two patients with schizophrenia that were absent in 600 control chromosomes. In our complementary mouse model studies, we identified a haploinsufficient effect of Rtn4r on locomotor activity, but normal performance in schizophrenia-related behavioral tasks. We also provide evidence that Rtn4r deficiency can modulate the long-term behavioral effects of transient postnatal N-methyl-D-aspartate (NMDA) receptor hypofunction. Conclusions. Our results do not support a major role of RTN4R in susceptibility to schizophrenia or the cognitive and behavioral deficits observed in individuals with 22q11 microdeletions. However, they suggest that RTN4R may modulate the genetic risk or clinical expression of schizophrenia in a subset of patients and identify additional studies that will be necessary to clarify the role of RTN4R in psychiatric phenotypes. In addition, our results raise interesting issues about evaluating the significance of rare genetic variants in disease and their role in causation. © 2007 Hsu et al.

Publication Title

PLoS ONE

Recommended Citation

Hsu, R., Woodroffe, A., Lai, W., Cook, M., Mukai, J., Dunning, J., Swanson, D., & Roos, J. (2007). Nogo receptor 1 (RTN4R) as a candidate gene for schizophrenia: Analysis using human and mouse genetic approaches. PLoS ONE, 2 (11) https://doi.org/10.1371/journal.pone.0001234