GWA study data mining and independent replication identify cardiomyopathy-associated 5 (CMYA5) as a risk gene for schizophrenia.
Chen X., Lee G., Maher BS., Fanous AH., Chen J., Zhao Z., Guo A., van den Oord E., Sullivan PF., Shi J., Levinson DF., Gejman PV., Sanders A., Duan J., Owen MJ., Craddock NJ., O'Donovan MC., Blackman J., Lewis D., Kirov GK., Qin W., Schwab S., Wildenauer D., Chowdari K., Nimgaonkar V., Straub RE., Weinberger DR., O'Neill FA., Walsh D., Bronstein M., Darvasi A., Lencz T., Malhotra AK., Rujescu D., Giegling I., Werge T., Hansen T., Ingason A., Nöethen MM., Rietschel M., Cichon S., Djurovic S., Andreassen OA., Cantor RM., Ophoff R., Corvin A., Morris DW., Gill M., Pato CN., Pato MT., Macedo A., Gurling HMD., McQuillin A., Pimm J., Hultman C., Lichtenstein P., Sklar P., Purcell SM., Scolnick E., St Clair D., Blackwood DHR., Kendler KS., GROUP investigators None., International Schizophrenia Consortium None.
We conducted data-mining analyses using the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE) and molecular genetics of schizophrenia genome-wide association study supported by the genetic association information network (MGS-GAIN) schizophrenia data sets and performed bioinformatic prioritization for all the markers with P-values ≤0.05 in both data sets. In this process, we found that in the CMYA5 gene, there were two non-synonymous markers, rs3828611 and rs10043986, showing nominal significance in both the CATIE and MGS-GAIN samples. In a combined analysis of both the CATIE and MGS-GAIN samples, rs4704591 was identified as the most significant marker in the gene. Linkage disequilibrium analyses indicated that these markers were in low LD (3 828 611-rs10043986, r(2)=0.008; rs10043986-rs4704591, r(2)=0.204). In addition, CMYA5 was reported to be physically interacting with the DTNBP1 gene, a promising candidate for schizophrenia, suggesting that CMYA5 may be involved in the same biological pathway and process. On the basis of this information, we performed replication studies for these three single-nucleotide polymorphisms. The rs3828611 was found to have conflicting results in our Irish samples and was dropped out without further investigation. The other two markers were verified in 23 other independent data sets. In a meta-analysis of all 23 replication samples (family samples, 912 families with 4160 subjects; case-control samples, 11 380 cases and 15 021 controls), we found that both markers are significantly associated with schizophrenia (rs10043986, odds ratio (OR)=1.11, 95% confidence interval (CI)=1.04-1.18, P=8.2 × 10(-4) and rs4704591, OR=1.07, 95% CI=1.03-1.11, P=3.0 × 10(-4)). The results were also significant for the 22 Caucasian replication samples (rs10043986, OR=1.11, 95% CI=1.03-1.17, P=0.0026 and rs4704591, OR=1.07, 95% CI=1.02-1.11, P=0.0015). Furthermore, haplotype conditioned analyses indicated that the association signals observed at these two markers are independent. On the basis of these results, we concluded that CMYA5 is associated with schizophrenia and further investigation of the gene is warranted.