Evidence for Shared Genetic Risk Between Methamphetamine-Induced Psychosis and Schizophrenia

被引:0
|
作者
Masashi Ikeda
Yuko Okahisa
Branko Aleksic
Mujun Won
Naoki Kondo
Nobuya Naruse
Kumi Aoyama-Uehara
Ichiro Sora
Masaomi Iyo
Ryota Hashimoto
Yoshiya Kawamura
Nao Nishida
Taku Miyagawa
Masatoshi Takeda
Tsukasa Sasaki
Katsushi Tokunaga
Norio Ozaki
Hiroshi Ujike
Nakao Iwata
机构
[1] Fujita Health University School of Medicine,Department of Psychiatry
[2] Okayama University Graduate School of Medicine,Department of Neuropsychiatry
[3] Dentistry and Pharmaceutical Sciences,Department of Psychiatry
[4] Nagoya University Graduate School of Medicine,Department of Biological Psychiatry
[5] Japanese Genetic Initiative for Drug Abuse (JGIDA),Department of Psychiatry
[6] Kojin Hospital,Department of Psychiatry
[7] Seimei Hospital,Department of Psychiatry
[8] Saitama Prefectural Psychiatric Hospital,Department of Human Genetics
[9] Serigaya Hospital,Graduate School of Education and Division for Counseling and Support
[10] Tohoku University Graduate School of Medicine,undefined
[11] Chiba University Graduate School of Medicine,undefined
[12] Osaka University Graduate School of Medicine,undefined
[13] Molecular Research Center for Children’s Mental Development,undefined
[14] United Graduate School of Child Development,undefined
[15] Osaka University,undefined
[16] Kanazawa University and Hamamatsu University School of Medicine,undefined
[17] Sakae Seijinkai Hospital,undefined
[18] Graduate School of Medicine,undefined
[19] The University of Tokyo,undefined
[20] The University of Tokyo,undefined
来源
Neuropsychopharmacology | 2013年 / 38卷
关键词
substance-induced psychosis; genome-wide association study; schizophrenia; methamphetamine; substance use disorder; polygenic component analysis;
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摘要
Methamphetamine (METH) use can provoke psychotic reactions requiring immediate treatment, namely METH-induced psychosis. Although the distinction between METH-induced and primary psychosis is important for understanding their clinical courses, we do not have clear diagnostic procedure by their symptoms. Not only are there similarities between the clinical features of METH-induced psychosis and schizophrenia (SCZ), but there is also epidemiological evidence of a shared genetic risk between ‘METH-related’ disorders and SCZ, which makes the differentiation of these two conditions difficult. In this study, we conducted a genome-wide association study (GWAS) targeting METH-dependent patients. The METH sample group, used in the METH-dependence GWAS, included 236 METH-dependent patients and 864 healthy controls. We also included a ‘within-case’ comparison between 194 METH-induced psychosis patients and 42 METH-dependent patients without psychosis in a METH-induced psychosis GWAS. To investigate the shared genetic components between METH dependence, METH-induced psychosis, and SCZ, data from our previous SCZ GWAS (total N=1108) were re-analyzed. In the SNP-based analysis, none of the SNPs showed genome-wide significance in either data set. By performing a polygenic component analysis, however, we found that a large number of ‘risk’ alleles for METH-induced psychosis are over-represented in individuals with SCZ (Pbest=0.0090). Conversely, we did not detect enrichment either between METH dependence and METH-induced psychosis or between METH dependence and SCZ. The results support previous epidemiological and neurobiological evidence for a relationship between METH-induced psychosis and SCZ. These also suggest that the overlap between genes scored as positive in these data sets can have higher probability as susceptibility genes for psychosis.
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页码:1864 / 1870
页数:6
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