Literature DB >> 21285144

After GWAS: searching for genetic risk for schizophrenia and bipolar disorder.

Elliot S Gershon1, Ney Alliey-Rodriguez, Chunyu Liu.   

Abstract

Ten years ago it was widely expected that the genetic basis of common disease would be resolved by genome-wide association studies (GWAS), large-scale studies in which the entire genome is covered by genetic markers. However, the bulk of heritable variance remains unexplained. The authors consider several alternative research strategies. For instance, whereas it has been hypothesized that a common disease is associated primarily with common genetic variants, it is now plausible that multiple rare variants each have a potent effect on disease risk and that they could accumulate to become a substantial component of common disease risk. This idea has become more appealing since the discovery that copy number variants (CNVs) are a substantial source of human mutations and are associated with multiple common diseases. CNVs are structural genomic variants consisting of microinsertions, microdeletions, and transpositions in the human genome. It has been argued that numerous rare CNVs are plausible causes of a substantial proportion of common disease, and rare CNVs have been found to be potent risk factors in schizophrenia and autism. Another approach is to "parse the genome," i.e., reanalyze subsets of current GWAS data, since the noise inherent in genome-wide approaches may be hiding valid associations. Lastly, technological advances and declining costs may allow large-scale genome-wide sequencing that would comprehensively identify all genetic variants. Study groups even larger than the 10,000 subjects in current meta-analyses would be required, but the outcomes may lead to resolution of our current dilemma in common diseases: Where is the missing heritability?

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Year:  2011        PMID: 21285144      PMCID: PMC6760656          DOI: 10.1176/appi.ajp.2010.10091340

Source DB:  PubMed          Journal:  Am J Psychiatry        ISSN: 0002-953X            Impact factor:   18.112


  72 in total

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5.  Genetic and childhood trauma interaction effect on age of onset in bipolar disorder: An exploratory analysis.

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6.  Identification of Distinct Psychosis Biotypes Using Brain-Based Biomarkers.

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Review 7.  Postmortem brain: an underutilized substrate for studying severe mental illness.

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Review 9.  Psychiatric disorders in toxoplasma seropositive patients--the CD8 connection.

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Review 10.  Confluence of genes, environment, development, and behavior in a post Genome-Wide Association Study world.

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