438 research outputs found
Identification of rare nonsynonymous variants in SYNE1/CPG2 in bipolar affective disorder
Background: Bipolar affective disorder (BPD) is a severe
mood disorder with a prevalence of ∼ 1.5% in the
population. The pathogenesis of BPD is poorly understood;
however, a strong heritable component has been identified.
Previous genome-wide association studies have indicated a
region on 6q25, coding for the SYNE1 gene, which increases
disease susceptibility. SYNE1 encodes the synaptic nuclear
envelope protein-1, nesprin-1. A brain-specific splice variant
of SYNE1, CPG2 encoding candidate plasticity gene 2, has
been identified. The intronic single-nucleotide
polymorphism with the strongest genome-wide significant
association in BPD, rs9371601, is present in both SYNE1
and CPG2. / Methods: We screened 937 BPD samples for genetic
variation in SYNE1 exons 14–33, which covers the CPG2
region, using high-resolution melt analysis. In addition, we
screened two regions of increased transcriptional activity,
one of them proposed to be the CPG2 promoter region. / Results and Conclusion: We identified six nonsynonymous
and six synonymous variants. We genotyped three rare
nonsynonymous variants, rs374866393, rs148346599 and
rs200629713, in a total of 1099 BPD samples and 1056
controls. Burden analysis of these rare variants did not show
a significant association with BPD. However, nine patients
are compound heterozygotes for variants in SYNE1/CPG2,
suggesting that rare coding variants may contribute
significantly towards the complex genetic architecture
underlying BPD. Imputation analysis in our own wholegenome
sequencing sample of 99 BPD individuals
identified an additional eight risk variants in the CPG2
region of SYNE1
Lost in the Storm: The Academic Collaborations that Went Missing in Hurricane Isaac
By exploiting the cancellation of the 2012 American Political Science Association Annual Meeting, we investigate the role of conferences in facilitating academic collaboration. We assembled datasets comprising 17,467 academics, and in difference-in-differences analysis we find that the conference cancellation led to a decrease in individuals' likelihood of co-authoring an article with another attendant by sixteen percent. Moreover, collaborations formed among attendants of (occurring) conferences are associated with more successful co-publications: an effect which is sharpest for teams that are new or non-collocated. Conferences seem to de-cluster the co-authorship network. Altogether, our findings demonstrate the importance of conferences in scientific production
Allelic Association, DNA Resequencing and Copy Number Variation at the Metabotropic Glutamate Receptor GRM7 Gene Locus in Bipolar Disorder
Genetic markers at the GRM7 gene have shown allelic association with bipolar disorder (BP) in several case-control samples including our own sample. In this report, we present results of resequencing the GRM7 gene in 32 bipolar samples and 32 random controls selected from 553 bipolar cases and 547 control samples (UCL1). Novel and potential etiological base pair changes discovered by resequencing were genotyped in the entire UCL case-control sample. We also report on the association between GRM7 and BP in a second sample of 593 patients and 642 controls (UCL2). The three most significantly associated SNPs in the original UCL1 BP GWAS sample were genotyped in the UCL2 sample, of which none were associated. After combining the genotype data for the two samples only two (rs1508724 and rs6769814) of the original three SNP markers remained significantly associated with BP. DNA sequencing revealed mutations in three cases which were absent in control subjects. A 3'-UTR SNP rs56173829 was found to be significantly associated with BP in the whole UCL sample (P = 0.035; OR = 0.482), the rare allele being less common in cases compared to controls. Bioinformatic analyses predicted a change in the centroid secondary structure of RNA and alterations in the miRNA binding sites for the mutated base of rs56173829. We also validated two deletions and a duplication within GRM7 using quantitative-PCR which provides further support for the pre-existing evidence that copy number variants at GRM7 may have a role in the etiology of BP. © 2014 The Authors. American Journal of Medical Genetics Part B: Neuropsychiatric Published by Wiley Periodicals, Inc
Characterising competitive equilibrium in terms of opportunity
This paper analyses alternative profiles of opportunity sets for individuals in an exchange economy, without assuming that individuals’ choices reveal coherent preferences. It introduces the concept of a ‘market-clearing single-price regime’, representing a profile of opportunity sets consistent with competitive equilibrium. It also proposes an opportunity-based normative criterion, the Strong Opportunity Criterion, which is analogous with the core in preference-based analysis. It shows that every market-clearing single-price regime satisfies the Strong Opportunity Criterion and that, in the limit as an economy is replicated, only such regimes have this property
Jet interactions with a giant molecular cloud in the Galactic centre and ejection of hypervelocity stars
The hypervelocity OB stars in the Milky Way Galaxy were ejected from the
central regions some 10-100 million years ago. We argue that these stars, {as
well as many more abundant bound OB stars in the innermost few parsecs,} were
generated by the interactions of an AGN jet from the central black hole with a
dense molecular cloud. Considerations of the associated energy and momentum
injection have broader implications for the possible origin of the Fermi
bubbles and for the enrichment of the intergalactic medium.Comment: 4 pages, 1 figure. Astronomy and Astrophysics Letters, in pres
Evidence for the association of the DAOA (G72) gene with schizophrenia and bipolar disorder but not for the association of the DAO gene with schizophrenia
Background: Previous linkage and association studies have implicated the D-amino acid oxidase activator gene (DAOA)/G30 locus or neighbouring region of chromosome 13q33.2 in the genetic susceptibility to both schizophrenia and bipolar disorder. Four single nucleotide polymorphisms (SNPs) within the D-amino acid oxidase (DAO) gene located at 12q24.11 have also been found to show allelic association with schizophrenia.Methods: We used the case control method to test for genetic association with variants at these loci in a sample of 431 patients with schizophrenia, 303 patients with bipolar disorder and 442 ancestrally matched supernormal controls all selected from the UK population.Results: Ten SNPs spanning the DAOA locus were genotyped in these samples. In addition three SNPs were genotyped at the DAO locus in the schizophrenia sample. Allelic association was detected between the marker rs3918342 (M23), 3' to the DAOA gene and both schizophrenia (chi(2) = 5.824 p = 0.016) and bipolar disorder (chi(2) = 4.293 p = 0.038). A trend towards association with schizophrenia was observed for two other DAOA markers rs3916967 (M14, chi(2) = 3.675 p = 0.055) and rs1421292 (M24; chi(2) = 3.499 p = 0.062). A test of association between a three marker haplotype comprising of the SNPs rs778293 (M22), rs3918342 (M23) and rs1421292 (M24) and schizophrenia gave a global empirical significance of p = 0.015. No evidence was found to confirm the association of genetic markers at the DAO gene with schizophrenia.Conclusion: Our results provide some support for a role for DAOA in susceptibility to schizophrenia and bipolar disorder
Genome-wide association study of antisocial personality disorder diagnostic criteria provides evidence for shared risk factors across disorders
INTRODUCTION: While progress has been made in determining the genetic basis of antisocial behaviour, little progress has been made for antisocial personality disorder (ASPD), a condition that often co-occurs with other psychiatric conditions including substance use disorders, attention deficit hyperactivity disorder (ADHD), and anxiety disorders. This study aims to improve the understanding of the genetic risk for ASPD and its relationship with other disorders and traits. METHODS: We conducted a genome-wide association study (GWAS) of the number of ASPD diagnostic criteria data from 3217 alcohol-dependent participants recruited in the UK (UCL, N = 644) and the USA (Yale-Penn, N = 2573). RESULTS: We identified rs9806493, a chromosome 15 variant, that showed a genome-wide significant association (Z-score = -5.501, P = 3.77 × 10-8) with ASPD criteria. rs9806493 is an eQTL for SLCO3A1 (Solute Carrier Organic Anion Transporter Family Member 3A1), a ubiquitously expressed gene with strong expression in brain regions that include the anterior cingulate and frontal cortices. Polygenic risk score analysis identified positive correlations between ASPD and smoking, ADHD, depression traits, and posttraumatic stress disorder. Negative correlations were observed between ASPD PRS and alcohol intake frequency, reproductive traits, and level of educational attainment. CONCLUSION: This study provides evidence for an association between ASPD risk and SLCO3A1 and provides insight into the genetic architecture and pleiotropic associations of ASPD
Genome-wide association study identifies 30 Loci Associated with Bipolar Disorder
Bipolar disorder is a highly heritable psychiatric disorder. We performed a genome-wide association study including 20,352 cases and 31,358 controls of European descent, with follow-up analysis of 822 variants with P\u3c1×10−4 in an additional 9,412 cases and 137,760 controls. Eight of the 19 variants that were genome-wide significant (GWS, p \u3c 5×10−8) in the discovery GWAS were not GWS in the combined analysis, consistent with small effect sizes and limited power but also with genetic heterogeneity. In the combined analysis 30 loci were GWS including 20 novel loci. The significant loci contain genes encoding ion channels, neurotransmitter transporters and synaptic components. Pathway analysis revealed nine significantly enriched gene-sets including regulation of insulin secretion and endocannabinoid signaling. BDI is strongly genetically correlated with schizophrenia, driven by psychosis, whereas BDII is more strongly correlated with major depressive disorder. These findings address key clinical questions and provide potential new biological mechanisms for BD
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