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The use of polygenic risk scores to identify phenotypes associated with genetic risk of schizophrenia: Systematic review.

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TLDR
Overall, SZ-PRS was associated with increased risk for psychiatric disorders such as depression and bipolar disorder, lower performance IQ and negative symptoms, and a framework is proposed to guide robust reporting of PRS associations in the future.
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This article is published in Schizophrenia Research.The article was published on 2017-11-10 and is currently open access. It has received 115 citations till now. The article focuses on the topics: Bipolar disorder & Schizophrenia.

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Citations
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Apparent latent structure within the UK Biobank sample has implications for epidemiological analysis

TL;DR: It is found that major health outcomes appear geographically structured and that coincident structure in health outcomes and genotype data can yield biased associations, and that fine-scale structure is detectable in apparently homogeneous samples such as ALSPAC when measured very precisely, and remains detectable in UK Biobank despite conventional approaches to account for it.
References
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Journal ArticleDOI

Genome-wide association study reveals greater polygenic loading for schizophrenia in cases with a family history of illness.

TL;DR: Familial illness might represent a more heritable form of schizophrenia, as suggested by previous epidemiological studies, and suggestive evidence of allelic effects detectable in large GWAS of schizophrenia that might be specific to particular family history subgroups is found.
Journal ArticleDOI

The relationship between schizophrenia and rheumatoid arthritis revisited: Genetic and epidemiological analyses

TL;DR: The current findings do not support the assertion that the relationship between RA and SCZ is explained by genetic factors, which appear to have little or no effect.
Journal ArticleDOI

Genomewide association analyses of electrophysiological endophenotypes for schizophrenia and psychotic bipolar disorders: a preliminary report.

TL;DR: Among patients with psychotic illness, PRS results indicated genetic overlap between SCZ loci and gamma oscillation and between BIP locus and P3 amplitude, and common variants associated with ERP endophenotypes are identified.
Journal ArticleDOI

Seasonality shows evidence for polygenic architecture and genetic correlation with schizophrenia and bipolar disorder.

TL;DR: The risk for schizophrenia and seasonality had the largest overlap, an unprecedented finding that requires replication in other populations and has potential clinical implications considering overlapping cognitive deficits in seasonal affective disorders and schizophrenia.
Journal ArticleDOI

Raising attention to attention deficit hyperactivity disorder in schizophrenia.

TL;DR: The complex relationship between stimulants use and psychotic symptoms is elucidated, discussing the potential role of ADHD medication in inducing psychosis or in exacerbating it, and the Research Domain Criteria approach might offer an interesting perspective for disentangling common circuits underpinning both disorders.
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Frequently Asked Questions (9)
Q1. What are the contributions mentioned in the paper "The use of polygenic risk scores to identify phenotypes associated with genetic risk of schizophrenia: systematic review" ?

This paper conducted a systematic review to identify studies that have used a polygenic risk score ( PRS ) approach to examine phenotypes associated with genetic risk for schizophrenia. 

One of the main advantages of the PRS approach is the ability to study how genetic risk for schizophrenia is manifest across the general population, and during different stages of development. 

Future increases in size of discovery samples may also enable PRSs to make a meaningful contribution to risk prediction models, as has been shown for some non-psychiatric disorders (Chatterjee et al. 2016). 

The population-based Longitudinal Experiences and Perceptions (LEAP) study found that SZPRS was associated with decreased anhedonia (strongest PT<0.5; one-tailed p=0.003) and parent-rated negative symptoms in adolescence (one-tailed p=0.029) (Sieradzka et al. 2014). 

The SZ-PRS was consistently associated with poorer cognition in population-based studies and from childhood through to older age (McIntosh et al. 2013; Hubbard et al. 2016). 

In the Netherlands case-control study of schizophrenia, SZ-PRS was associated with five symptom dimensions (strongest PT<0.5): positive (p=<0.01), negative (p= <0.001), mania (p= <0.01), depression (p= <0.001) and disorganisation (p=0.04) within the combined casecontrol sample, but not with these dimensions in cases and controls examined separately (Derks et al. 2012). 

the inconsistency of reporting of results across studies meant that only a narrative approach to this review was feasible, and assessment of publication bias was not possible. 

The SZ-PRS was also associated with a number of other, non-psychiatric outcomes, including diabetes, RA and CD (Stringer et al. 2014), though results were not consistent across studies. 

Higher SZ-PRS was associated with lower total IQ in a combined schizophrenia case–control sample (strongest PT<0.3, p=8x10-4), but this was attenuated when analysing cases only (p=0.067), with no association in controls (van Scheltinga et al. 2013).