Updates are available Addendum dated 2016-08-01
Click to view Addendum: https://doi.org/10.1038/nn0816-1115c
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Authors
Siegert, Sandra
Seo, Jinsoo
Kwon, Ester J
Rudenko, Andrii
Cho, Sukhee
Wang, Wenyuan
Flood, Zachary
Martorell, Anthony J
Ericsson, Maria
Mungenast, Alison E
Tsai, Li-Huei
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Article History
Received: 16 February 2015
Accepted: 24 April 2015
First Online: 25 May 2015
Change Date: 8 July 2016
Change Type: Update
Change Details: It has come to our attention that our results, as presented, have caused some confusion among readers with regard to genetic variation at the MIR137 locus, gene expression of MIR137 and schizophrenia risk. It should be noted that it is currently unclear how gene variants at the MIR137 locus confers disease risk and which are the causative or functional alleles or the gene(s) that mediate risk. Also, it is not clear to what extent a single disease-associated SNP, in isolation, relates to disease. In our study we did not examine the effects of single alleles since they often segregate together. It remains to be determined how the multiple reported disease-associated SNPs in the MIR137 locus alone and in combination influence gene expression. To clarify this would require genome editing to alter SNPs, one by one, in cell lines. Finally, further studies are required to determine whether the synaptic and behavioral changes observed in this study can be linked to the specific genetic variants within the MIR137 locus associated with schizophrenia in genome-wide association studies.
Competing interests
: The authors declare no competing financial interests.
