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4. Transferability of Ancestry‐Specific and Cross‐Ancestry CYP2A6 Activity Genetic Risk Scores in African and European Populations

Author

El‐Boraie, Ahmed, Chenoweth, Meghan J, Pouget, Jennie G, Benowitz, Neal L, Fukunaga, Koya, Mushiroda, Taisei, Kubo, Michiaki, Nollen, Nicole L, Cox, Lisa Sanderson, Lerman, Caryn, Knight, Jo, and Tyndale, Rachel F

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Genetics, Tobacco, Tobacco Smoke and Health, Clinical Research, Respiratory, Cardiovascular, Cancer, Good Health and Well Being, Adult, Black or African American, Black People, Cotinine, Cytochrome P-450 CYP2A6, Female, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Pharmacogenomic Variants, Principal Component Analysis, Risk Factors, Smoking, Smoking Cessation, Treatment Outcome, White People, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences
Abstract

The Nicotine Metabolite Ratio (NMR; 3-hydroxycotinine/cotinine), a highly heritable index of nicotine metabolic inactivation by the CYP2A6 enzyme, is associated with numerous smoking behaviors and diseases, as well as unique cessation outcomes. However, the NMR cannot be measured in nonsmokers, former smokers, or intermittent smokers, for example, in evaluating tobacco-related disease risk. Traditional pharmacogenetic groupings based on CYP2A6 * alleles capture a modest portion of NMR variation. We previously created a CYP2A6 weighted genetic risk score (wGRS) for European (EUR)-ancestry populations by incorporating independent signals from genome-wide association studies to capture a larger proportion of NMR variation. However, CYP2A6 genetic architecture is unique to ancestral populations. In this study, we developed and replicated an African-ancestry (AFR) wGRS, which captured 30-35% of the variation in NMR. We demonstrated model robustness against known environmental sources of NMR variation. Furthermore, despite the vast diversity within AFR populations, we showed that the AFR wGRS was consistent between different US geographical regions and unaltered by fine AFR population substructure. The AFR and EUR wGRSs can distinguish slow from normal metabolizers in their respective populations, and were able to reflect unique smoking cessation pharmacotherapy outcomes previously observed for the NMR. Additionally, we evaluated the utility of a cross-ancestry wGRS, and the capacity of EUR, AFR, and cross-ancestry wGRSs to predict the NMR within stratified or admixed AFR-EUR populations. Overall, our findings establish the clinical benefit of applying ancestry-specific wGRSs, demonstrating superiority of the AFR wGRS in AFRs.

Published
2021

7. Associating CYP2A6 structural variants with ovarian and lung cancer risk in the UK Biobank : replication and extension

Author

Langlois, Alec W. R., Pouget, Jennie G., Knight, Jo, Chenoweth, Meghan J., Tyndale, Rachel F., Langlois, Alec W. R., Pouget, Jennie G., Knight, Jo, Chenoweth, Meghan J., and Tyndale, Rachel F.

Abstract

CYP2A6 is a polymorphic enzyme that inactivates nicotine; structural variants (SVs) include gene deletions and hybrids with the neighboring pseudogene CYP2A7. Two studies found that CYP2A7 deletions were associated with ovarian cancer risk. Using their methodology, we aimed to characterize CYP2A6 SVs (which may be misidentified by prediction software as CYP2A7 SVs), then assess CYP2A6 SV-associated risk for ovarian cancer, and extend analyses to lung cancer. An updated reference panel was created to impute CYP2A6 SVs from UK Biobank array data. Logistic regression models analyzed the association between CYP2A6 SVs and cancer risk, adjusting for covariates. Software-predicted CYP2A7 deletions were concordant with known CYP2A6 SVs. Deleterious CYP2A6 SVs were not associated with ovarian cancer (OR = 1.06; 95% CI: 0.80-1.37; p = 0.7) but did reduce the risk of lung cancer (OR = 0.44; 95% CI: 0.29-0.64; p

Published
2024

8. CYP2A6 associates with respiratory disease risk and younger age of diagnosis : a phenome-wide association Mendelian randomization study

Author

Giratallah, Haidy, Chenoweth, Meghan J, Pouget, Jennie G, El-Boraie, Ahmed, Alsaafin, Alaa, Lerman, Caryn, Knight, Jo, Tyndale, Rachel F, Giratallah, Haidy, Chenoweth, Meghan J, Pouget, Jennie G, El-Boraie, Ahmed, Alsaafin, Alaa, Lerman, Caryn, Knight, Jo, and Tyndale, Rachel F

Abstract

CYP2A6, a genetically variable enzyme, inactivates nicotine, activates carcinogens, and metabolizes many pharmaceuticals. Variation in CYP2A6 influences smoking behaviors and tobacco-related disease risk. This phenome-wide association study examined associations between a reconstructed version of our weighted genetic risk score (wGRS) for CYP2A6 activity with diseases in the UK Biobank (N = 395 887). Causal effects of phenotypic CYP2A6 activity (measured as the nicotine metabolite ratio: 3′-hydroxycotinine/cotinine) on the phenome-wide significant (PWS) signals were then estimated in two-sample Mendelian Randomization using the wGRS as the instrument. Time-to-diagnosis age was compared between faster versus slower CYP2A6 metabolizers for the PWS signals in survival analyses. In the total sample, six PWS signals were identified: two lung cancers and four obstructive respiratory diseases PheCodes, where faster CYP2A6 activity was associated with greater disease risk (Ps < 1 × 10−6). A significant CYP2A6-by-smoking status interaction was found (Psinteraction < 0.05); in current smokers, the same six PWS signals were found as identified in the total group, whereas no PWS signals were found in former or never smokers. In the total sample and current smokers, CYP2A6 activity causal estimates on the six PWS signals were significant in Mendelian Randomization (Ps < 5 × 10−5). Additionally, faster CYP2A6 metabolizer status was associated with younger age of disease diagnosis for the six PWS signals (Ps < 5 × 10−4, in current smokers). These findings support a role for faster CYP2A6 activity as a causal risk factor for lung cancers and obstructive respiratory diseases among current smokers, and a younger onset of these diseases. This research utilized the UK Biobank Resource.

Published
2024

9. Analysis of five chronic inflammatory diseases identifies 27 new associations and highlights disease-specific patterns at shared loci

Author

Ellinghaus, David, Jostins, Luke, Spain, Sarah L, Cortes, Adrian, Bethune, Jörn, Han, Buhm, Park, Yu Rang, Raychaudhuri, Soumya, Pouget, Jennie G, Hübenthal, Matthias, Folseraas, Trine, Wang, Yunpeng, Esko, Tonu, Metspalu, Andres, Westra, Harm-Jan, Franke, Lude, Pers, Tune H, Weersma, Rinse K, Collij, Valerie, D'Amato, Mauro, Halfvarson, Jonas, Jensen, Anders Boeck, Lieb, Wolfgang, Degenhardt, Franziska, Forstner, Andreas J, Hofmann, Andrea, Schreiber, Stefan, Mrowietz, Ulrich, Juran, Brian D, Lazaridis, Konstantinos N, Brunak, Søren, Dale, Anders M, Trembath, Richard C, Weidinger, Stephan, Weichenthal, Michael, Ellinghaus, Eva, Elder, James T, Barker, Jonathan NWN, Andreassen, Ole A, McGovern, Dermot P, Karlsen, Tom H, Barrett, Jeffrey C, Parkes, Miles, Brown, Matthew A, and Franke, Andre

Subjects
Biological Sciences, Genetics, Prevention, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Bayes Theorem, Cholangitis, Sclerosing, Chronic Disease, Colitis, Ulcerative, Comorbidity, Crohn Disease, Genetic Heterogeneity, Genetic Pleiotropy, Genetic Variation, Genome-Wide Association Study, Genotype, Humans, Inflammation, Psoriasis, Quantitative Trait Loci, Spondylitis, Ankylosing, International IBD Genetics Consortium, International Genetics of Ankylosing Spondylitis Consortium, International PSC Study Group, Genetic Analysis of Psoriasis Consortium, Psoriasis Association Genetics Extension, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology
Abstract

We simultaneously investigated the genetic landscape of ankylosing spondylitis, Crohn's disease, psoriasis, primary sclerosing cholangitis and ulcerative colitis to investigate pleiotropy and the relationship between these clinically related diseases. Using high-density genotype data from more than 86,000 individuals of European ancestry, we identified 244 independent multidisease signals, including 27 new genome-wide significant susceptibility loci and 3 unreported shared risk loci. Complex pleiotropy was supported when contrasting multidisease signals with expression data sets from human, rat and mouse together with epigenetic and expressed enhancer profiles. The comorbidities among the five immune diseases were best explained by biological pleiotropy rather than heterogeneity (a subgroup of cases genetically identical to those with another disease, possibly owing to diagnostic misclassification, molecular subtypes or excessive comorbidity). In particular, the strong comorbidity between primary sclerosing cholangitis and inflammatory bowel disease is likely the result of a unique disease, which is genetically distinct from classical inflammatory bowel disease phenotypes.

Published
2016

15. Heart rate variability: Evaluating a potential biomarker of anxiety disorders.

Author

Tomasi, Julia, Zai, Clement C., Pouget, Jennie G., Tiwari, Arun K., and Kennedy, James L.

Subjects
HEART beat, ANXIETY disorders, GENETIC risk score, PARASYMPATHETIC nervous system, SYMPATHETIC nervous system, ANXIETY treatment
Abstract

Establishing quantifiable biological markers associated with anxiety will increase the objectivity of phenotyping and enhance genetic research of anxiety disorders. Heart rate variability (HRV) is a physiological measure reflecting the dynamic relationship between the sympathetic and parasympathetic nervous systems, and is a promising target for further investigation. This review summarizes evidence evaluating HRV as a potential physiological biomarker of anxiety disorders by highlighting literature related to anxiety and HRV combined with investigations of endophenotypes, neuroimaging, treatment response, and genetics. Deficient HRV shows promise as an endophenotype of pathological anxiety and may serve as a noninvasive index of prefrontal cortical control over the amygdala, and potentially aid with treatment outcome prediction. We propose that the genetics of HRV can be used to enhance the understanding of the genetics of pathological anxiety for etiological investigations and treatment prediction. Given the anxiety–HRV link, strategies are offered to advance genetic analytical approaches, including the use of polygenic methods, wearable devices, and pharmacogenetic study designs. Overall, HRV shows promising support as a physiological biomarker of pathological anxiety, potentially in a transdiagnostic manner, with the heart–brain entwinement providing a novel approach to advance anxiety treatment development. This review proposes that the genetics of heart rate variability (HRV) can be used to identify novel treatment targets for anxiety disorders given that impaired HRV has support as an anxiety endophenotype, reflects anxiety‐related brain activation patterns, and may predict treatment response. Advanced approaches such as use of wearables to collect large samples, polygenic risk score methods, and pharmacogenetics are suggested to develop HRV genetic research. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Genotyping, characterization, and imputation of known and novel CYP2A6 structural variants using SNP array data

Author

Langlois, Alec W R, El-Boraie, Ahmed, Pouget, Jennie G, Cox, Lisa Sanderson, Ahluwalia, Jasjit S, Fukunaga, Koya, Mushiroda, Taisei, Knight, Jo, Chenoweth, Meghan J, Tyndale, Rachel F, Langlois, Alec W R, El-Boraie, Ahmed, Pouget, Jennie G, Cox, Lisa Sanderson, Ahluwalia, Jasjit S, Fukunaga, Koya, Mushiroda, Taisei, Knight, Jo, Chenoweth, Meghan J, and Tyndale, Rachel F

Abstract

CYP2A6 metabolically inactivates nicotine. Faster CYP2A6 activity is associated with heavier smoking and higher lung cancer risk. The CYP2A6 gene is polymorphic, including functional structural variants (SV) such as gene deletions (CYP2A6*4), duplications (CYP2A6*1 × 2), and hybrids with the CYP2A7 pseudogene (CYP2A6*12, CYP2A6*34). SVs are challenging to genotype due to their complex genetic architecture. Our aims were to develop a reliable protocol for SV genotyping, functionally phenotype known and novel SVs, and investigate the feasibility of CYP2A6 SV imputation from SNP array data in two ancestry populations. European- (EUR; n = 935) and African- (AFR; n = 964) ancestry individuals from smoking cessation trials were genotyped for SNPs using an Illumina array and for CYP2A6 SVs using Taqman copy number (CN) assays. SV-specific PCR amplification and Sanger sequencing was used to characterize a novel SV. Individuals with SVs were phenotyped using the nicotine metabolite ratio, a biomarker of CYP2A6 activity. SV diplotype and SNP array data were integrated and phased to generate ancestry-specific SV reference panels. Leave-one-out cross-validation was used to investigate the feasibility of CYP2A6 SV imputation. A minimal protocol requiring three Taqman CN assays for CYP2A6 SV genotyping was developed and known SV associations with activity were replicated. The first domain swap CYP2A6-CYP2A7 hybrid SV, CYP2A6*53, was identified, sequenced, and associated with lower CYP2A6 activity. In both EURs and AFRs, most SV alleles were identified using imputation (>70% and >60%, respectively); importantly, false positive rates were <1%. These results confirm that CYP2A6 SV imputation can identify most SV alleles, including a novel SV.

Published
2023

17. Fine-mapping the CYP2A6regional association with nicotine metabolism among African American smokers

Author

Pouget, Jennie G., Giratallah, Haidy, Langlois, Alec W. R., El-Boraie, Ahmed, Lerman, Caryn, Knight, Jo, Cox, Lisa Sanderson, Nollen, Nikki L., Ahluwalia, Jasjit S., Benner, Christian, Chenoweth, Meghan J., and Tyndale, Rachel F.

Abstract

The nicotine metabolite ratio (NMR; 3’hydroxycotinine/cotinine) is a stable biomarker for CYP2A6 enzyme activity and nicotine clearance, with demonstrated clinical utility in personalizing smoking cessation treatment. Common genetic variation in the CYP2A6region is strongly associated with NMR in smokers. Here, we investigated this regional association in more detail. We evaluated the association of CYP2A6single-nucleotide polymorphisms (SNPs) and * alleles with NMR among African American smokers (N = 953) from two clinical trials of smoking cessation. Stepwise conditional analysis and Bayesian fine-mapping were undertaken. Putative causal variants were incorporated into an existing African ancestry-specific genetic risk score (GRS) for NMR, and the performance of the updated GRS was evaluated in both African American (n = 953) and European ancestry smokers (n = 933) from these clinical trials. Five independent associations with NMR in the CYP2A6region were identified using stepwise conditional analysis, including the deletion variant CYP2A6*4(beta = −0.90, p = 1.55 × 10−11). Six putative causal variants were identified using Bayesian fine-mapping (posterior probability, PP = 0.67), with the top causal configuration including CYP2A6*4, rs116670633, CYP2A6*9, rs28399451, rs8192720, and rs10853742 (PP = 0.09). Incorporating these putative causal variants into an existing ancestry-specific GRS resulted in comparable prediction of NMR within African American smokers, and improved trans-ancestry portability of the GRS to European smokers. Our findings suggest that both * alleles and SNPs underlie the association of the CYP2A6region with NMR among African American smokers, identify a shortlist of variants that may causally influence nicotine clearance, and suggest that portability of GRSs across populations can be improved through inclusion of putative causal variants.

Published
2024
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19. Genotyping, characterization, and imputation of known and novel CYP2A6structural variants using SNP array data

Author

Langlois, Alec W. R., El-Boraie, Ahmed, Pouget, Jennie G., Cox, Lisa Sanderson, Ahluwalia, Jasjit S., Fukunaga, Koya, Mushiroda, Taisei, Knight, Jo, Chenoweth, Meghan J., and Tyndale, Rachel F.

Abstract

CYP2A6 metabolically inactivates nicotine. Faster CYP2A6 activity is associated with heavier smoking and higher lung cancer risk. The CYP2A6gene is polymorphic, including functional structural variants (SV) such as gene deletions (CYP2A6*4), duplications (CYP2A6*1×2), and hybrids with the CYP2A7pseudogene (CYP2A6*12, CYP2A6*34). SVs are challenging to genotype due to their complex genetic architecture. Our aims were to develop a reliable protocol for SV genotyping, functionally phenotype known and novel SVs, and investigate the feasibility of CYP2A6SV imputation from SNP array data in two ancestry populations. European- (EUR; n= 935) and African- (AFR; n= 964) ancestry individuals from smoking cessation trials were genotyped for SNPs using an Illumina array and for CYP2A6SVs using Taqman copy number (CN) assays. SV-specific PCR amplification and Sanger sequencing was used to characterize a novel SV. Individuals with SVs were phenotyped using the nicotine metabolite ratio, a biomarker of CYP2A6 activity. SV diplotype and SNP array data were integrated and phased to generate ancestry-specific SV reference panels. Leave-one-out cross-validation was used to investigate the feasibility of CYP2A6SV imputation. A minimal protocol requiring three Taqman CN assays for CYP2A6SV genotyping was developed and known SV associations with activity were replicated. The first domain swap CYP2A6-CYP2A7hybrid SV, CYP2A6*53, was identified, sequenced, and associated with lower CYP2A6 activity. In both EURs and AFRs, most SV alleles were identified using imputation (>70% and >60%, respectively); importantly, false positive rates were <1%. These results confirm that CYP2A6SV imputation can identify most SV alleles, including a novel SV.

Published
2023
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21. Investigation of TSPO variants in schizophrenia and antipsychotic treatment outcomes

Author

Pouget, Jennie G, Gonçalves, Vanessa F, Nurmi, Erika L, Laughlin, Christopher P, Mallya, Karyn S, McCracken, James T, Aman, Michael G, McDougle, Christopher J, Scahill, Lawrence, Misener, Virginia L, Tiwari, Arun K, Zai, Clement C, Brandl, Eva J, Felsky, Daniel, Leung, Amy Q, Lieberman, Jeffrey A, Meltzer, Herbert Y, Potkin, Steven G, Niedling, Charlotte, Steimer, Werner, Leucht, Stefan, Knight, Jo, Müller, Daniel J, and Kennedy, James L

Published
2015
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23. Transferability Of Ancestry-Specific And Cross-Ancestry CYP2A6 Activity Genetic Risk Scores In African And European Populations

Author

El-Boraie, Ahmed, Chenoweth, Meghan J, Pouget, Jennie G, Benowitz, Neal L, Fukunaga, Koya, Mushiroda, Taisei, Kubo, Michiaki, Nollen, Nicole L, Cox, Lisa Sanderson, Lerman, Caryn, Knight, Jo, Tyndale, Rachel F, El-Boraie, Ahmed, Chenoweth, Meghan J, Pouget, Jennie G, Benowitz, Neal L, Fukunaga, Koya, Mushiroda, Taisei, Kubo, Michiaki, Nollen, Nicole L, Cox, Lisa Sanderson, Lerman, Caryn, Knight, Jo, and Tyndale, Rachel F

Abstract

The Nicotine Metabolite Ratio (NMR, 3-hydroxycotinine/cotinine), a highly heritable index of nicotine metabolic inactivation by the CYP2A6 enzyme, is associated with numerous smoking behaviors and diseases, as well as unique cessation outcomes. However, the NMR cannot be measured in non-, former- or intermittent-smokers, for example in evaluating tobacco-related disease risk. Traditional pharmacogenetic groupings based on CYP2A6 * alleles capture a modest portion of NMR variation. We previously created a CYP2A6 weighted genetic risk score (wGRS) for European-ancestry populations (EUR) by incorporating independent signals from genome-wide association studies to capture a larger proportion of NMR variation. However, CYP2A6 genetic architecture is unique to ancestral populations. In this study we developed and replicated an African-ancestry (AFR) wGRS which captured 30-35% of the variation in NMR. We demonstrated model robustness against known environmental sources of NMR variation. Furthermore, despite the vast diversity within AFR populations, we showed that the AFR wGRS was consistent between different US geographical regions and unaltered by fine AFR population substructure. The AFR and EUR wGRSs can distinguish slow from normal metabolizers in their respective populations, and were able to reflect unique smoking cessation pharmacotherapy outcomes previously observed for the NMR. Additionally, we evaluated the utility of a cross-ancestry wGRS, and the capacity of EUR, AFR, and cross-ancestry wGRSs to predict the NMR within stratified or admixed AFR-EUR populations. Overall, our findings establish the clinical benefit of applying ancestry-specific wGRSs, demonstrating superiority of the AFR wGRS in AFRs.

Published
2021

24. Associating CYP2A6structural variants with ovarian and lung cancer risk in the UK Biobank: replication and extension

Author

Langlois, Alec W. R., Pouget, Jennie G., Knight, Jo, Chenoweth, Meghan J., and Tyndale, Rachel F.

Abstract

CYP2A6 is a polymorphic enzyme that inactivates nicotine; structural variants (SVs) include gene deletions and hybrids with the neighboring pseudogene CYP2A7. Two studies found that CYP2A7deletions were associated with ovarian cancer risk. Using their methodology, we aimed to characterize CYP2A6SVs (which may be misidentified by prediction software as CYP2A7SVs), then assess CYP2A6SV-associated risk for ovarian cancer, and extend analyses to lung cancer. An updated reference panel was created to impute CYP2A6SVs from UK Biobank array data. Logistic regression models analyzed the association between CYP2A6SVs and cancer risk, adjusting for covariates. Software-predicted CYP2A7deletions were concordant with known CYP2A6SVs. Deleterious CYP2A6SVs were not associated with ovarian cancer (OR = 1.06; 95% CI: 0.80–1.37; p = 0.7) but did reduce the risk of lung cancer (OR = 0.44; 95% CI: 0.29–0.64; p < 0.0001), and a lung cancer subtype. Replication of known lung cancer associations indicates the validity of array-based SV analyses.

Published
2023
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25. Investigating the Causal Relationship of C-Reactive Protein with 32 Complex Somatic and Psychiatric Outcomes: A Large-Scale Cross-Consortium Mendelian Randomization Study

Author

Prins, Bram. P., Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E., Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P., Valdes, Ana M., Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D., Tsoi, Lam C., Evangelou, Evangelos, Nair, Rajan P., Grant, Struan F. A., Polychronakos, Constantin, Radstake, Timothy R. D., van Heel, David A., Dunstan, Melanie L., Wood, Nicholas W., Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S., Elder, James T., Knight, Jo, Arking, Dan E., Spector, Timothy D., Koeleman, Bobby P. C., van Duijn, Cornelia M., Martin, Javier, Morris, Andrew P., Weersma, Rinse K., Wijmenga, Cisca, Munroe, Patricia B., Perry, John R. B., Pouget, Jennie G., Jamshidi, Yalda, Snieder, Harold, and Alizadeh, Behrooz Z.

Subjects
Mental disorders -- Risk factors -- Research, Outcome and process assessment (Medical care) -- Analysis, C-reactive protein -- Investigations -- Analysis -- Research, Biological sciences
Abstract

Background C-reactive protein (CRP) is associated with immune, cardiometabolic, and psychiatric traits and diseases. Yet it is inconclusive whether these associations are causal. Methods and Findings We performed Mendelian randomization (MR) analyses using two genetic risk scores (GRSs) as instrumental variables (IVs). The first GRS consisted of four single nucleotide polymorphisms (SNPs) in the CRP gene (GRS.sub.CRP ), and the second consisted of 18 SNPs that were significantly associated with CRP levels in the largest genome-wide association study (GWAS) to date (GRS.sub.GWAS). To optimize power, we used summary statistics from GWAS consortia and tested the association of these two GRSs with 32 complex somatic and psychiatric outcomes, with up to 123,865 participants per outcome from populations of European ancestry. We performed heterogeneity tests to disentangle the pleiotropic effect of IVs. A Bonferroni-corrected significance level of less than 0.0016 was considered statistically significant. An observed p-value equal to or less than 0.05 was considered nominally significant evidence for a potential causal association, yet to be confirmed. The strengths (F-statistics) of the IVs were 31.92-3,761.29 and 82.32-9,403.21 for GRS.sub.CRP and GRS.sub.GWAS, respectively. CRP GRS.sub.GWAS showed a statistically significant protective relationship of a 10% genetically elevated CRP level with the risk of schizophrenia (odds ratio [OR] 0.86 [95% CI 0.79-0.94]; p < 0.001). We validated this finding with individual-level genotype data from the schizophrenia GWAS (OR 0.96 [95% CI 0.94-0.98]; p < 1.72 x 10.sup.-6). Further, we found that a standardized CRP polygenic risk score (CRP.sub.PRS) at p-value thresholds of 1 x 10.sup.-4, 0.001, 0.01, 0.05, and 0.1 using individual-level data also showed a protective effect (OR < 1.00) against schizophrenia; the first CRP.sub.PRS (built of SNPs with p < 1 x 10.sup.-4) showed a statistically significant (p < 2.45 x 10.sup.-4) protective effect with an OR of 0.97 (95% CI 0.95-0.99). The CRP GRS.sub.GWAS showed that a 10% increase in genetically determined CRP level was significantly associated with coronary artery disease (OR 0.88 [95% CI 0.84-0.94]; p < 2.4 x 10.sup.-5) and was nominally associated with the risk of inflammatory bowel disease (OR 0.85 [95% CI 0.74-0.98]; p < 0.03), Crohn disease (OR 0.81 [95% CI 0.70-0.94]; p < 0.005), psoriatic arthritis (OR 1.36 [95% CI 1.00-1.84]; p < 0.049), knee osteoarthritis (OR 1.17 [95% CI 1.01-1.36]; p < 0.04), and bipolar disorder (OR 1.21 [95% CI 1.05-1.40]; p < 0.007) and with an increase of 0.72 (95% CI 0.11-1.34; p < 0.02) mm Hg in systolic blood pressure, 0.45 (95% CI 0.06-0.84; p < 0.02) mm Hg in diastolic blood pressure, 0.01 ml/min/1.73 m.sup.2 (95% CI 0.003-0.02; p < 0.005) in estimated glomerular filtration rate from serum creatinine, 0.01 g/dl (95% CI 0.0004-0.02; p < 0.04) in serum albumin level, and 0.03 g/dl (95% CI 0.008-0.05; p < 0.009) in serum protein level. However, after adjustment for heterogeneity, neither GRS showed a significant effect of CRP level (at p < 0.0016) on any of these outcomes, including coronary artery disease, nor on the other 20 complex outcomes studied. Our study has two potential limitations: the limited variance explained by our genetic instruments modeling CRP levels in blood and the unobserved bias introduced by the use of summary statistics in our MR analyses. Conclusions Genetically elevated CRP levels showed a significant potentially protective causal relationship with risk of schizophrenia. We observed nominal evidence at an observed p < 0.05 using either GRS.sub.CRP or GRS.sub.GWAS -with persistence after correction for heterogeneity-for a causal relationship of elevated CRP levels with psoriatic osteoarthritis, rheumatoid arthritis, knee osteoarthritis, systolic blood pressure, diastolic blood pressure, serum albumin, and bipolar disorder. These associations remain yet to be confirmed. We cannot verify any causal effect of CRP level on any of the other common somatic and neuropsychiatric outcomes investigated in the present study. This implies that interventions that lower CRP level are unlikely to result in decreased risk for the majority of common complex outcomes., Author(s): Bram. P. Prins 1,2,*, Ali Abbasi 1,3,4, Anson Wong 5,6, Ahmad Vaez 1,7, Ilja Nolte 1, Nora Franceschini 8, Philip E. Stuart 9, Javier Guterriez Achury 10, Vanisha Mistry [...]

Published
2016
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26. Cross-disorder analysis of schizophrenia and 19 immune-mediated diseases identifies shared genetic risk

Author

Pouget, Jennie G, Han, Buhm, Wu, Yang, Mignot, Emmanuel, Ollila, Hanna M, Barker, Jonathan, Spain, Sarah, Dand, Nick, Trembath, Richard, Martin, Javier, Mayes, Maureen D, Bossini-Castillo, Lara, López-Isac, Elena, Jin, Ying, Santorico, Stephanie A, Spritz, Richard A, Hakonarson, Hakon, Polychronakos, Constantin, Raychaudhuri, Soumya, Knight, Jo, Schizophrenia Working Group of the Psychiatric Genomics Consorti, Pouget, Jennie G, Han, Buhm, Wu, Yang, Mignot, Emmanuel, Ollila, Hanna M, Barker, Jonathan, Spain, Sarah, Dand, Nick, Trembath, Richard, Martin, Javier, Mayes, Maureen D, Bossini-Castillo, Lara, López-Isac, Elena, Jin, Ying, Santorico, Stephanie A, Spritz, Richard A, Hakonarson, Hakon, Polychronakos, Constantin, Raychaudhuri, Soumya, Knight, Jo, and Schizophrenia Working Group of the Psychiatric Genomics Consorti

Abstract

Many immune diseases occur at different rates among people with schizophrenia compared to the general population. Here, we evaluated whether this phenomenon might be explained by shared genetic risk factors. We used data from large genome-wide association studies to compare the genetic architecture of schizophrenia to 19 immune diseases. First, we evaluated the association with schizophrenia of 581 variants previously reported to be associated with immune diseases at genome-wide significance. We identified five variants with potentially pleiotropic effects. While colocalization analyses were inconclusive, functional characterization of these variants provided the strongest evidence for a model in which genetic variation at rs1734907 modulates risk of schizophrenia and Crohn's disease via altered methylation and expression of EPHB4-a gene whose protein product guides the migration of neuronal axons in the brain and the migration of lymphocytes towards infected cells in the immune system. Next, we investigated genome-wide sharing of common variants between schizophrenia and immune diseases using cross-trait LD score regression. Of the 11 immune diseases with available genome-wide summary statistics, we observed genetic correlation between six immune diseases and schizophrenia: inflammatory bowel disease (rg = 0.12 ± 0.03, P = 2.49 × 10-4), Crohn's disease (rg = 0.097 ± 0.06, P = 3.27 × 10-3), ulcerative colitis (rg = 0.11 ± 0.04, P = 4.05 × 10-3), primary biliary cirrhosis (rg = 0.13 ± 0.05, P = 3.98 × 10-3), psoriasis (rg = 0.18 ± 0.07, P = 7.78 × 10-3) and systemic lupus erythematosus (rg = 0.13 ± 0.05, P = 3.76 × 10-3). With the exception of ulcerative colitis, the degree and direction of these genetic correlations were consistent with the expected phenotypic correlation based on epidemiological data. Our findings suggest shared genetic risk factors contribute to the epidemiological association of certain immune diseases and schizophrenia.

Published
2019

27. Association Study of the Complement Component C4 Gene in Tardive Dyskinesia

Author

Zai, Clement C., primary, Tiwari, Arun K., additional, Zai, Gwyneth C., additional, Freeman, Natalie, additional, Pouget, Jennie G., additional, Greco, James, additional, Tampakeras, Maria, additional, Shaikh, Sajid A., additional, Herbert, Deanna, additional, Emmerson, Heather, additional, Cheema, Sheraz Y., additional, Braganza, Nicole, additional, Müller, Daniel J., additional, Voineskos, Aristotle N., additional, Remington, Gary, additional, and Kennedy, James L., additional

Published
2019
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29. A Comprehensive Analysis of Nuclear-Encoded Mitochondrial Genes in Schizophrenia

Author

Goncalves, Vanessa F., Cappi, Carolina, Hagen, Christian M., Sequeira, Adolfo, Vawter, Marquis P., Derkach, Andriy, Zai, Clement C., Hedley, Paula L., Bybjerg-Grauholm, Jonas, Pouget, Jennie G., Cuperfain, Ari B., Sullivan, Patrick F., Christiansen, Michael, Kennedy, James L., Sun, Lei, Goncalves, Vanessa F., Cappi, Carolina, Hagen, Christian M., Sequeira, Adolfo, Vawter, Marquis P., Derkach, Andriy, Zai, Clement C., Hedley, Paula L., Bybjerg-Grauholm, Jonas, Pouget, Jennie G., Cuperfain, Ari B., Sullivan, Patrick F., Christiansen, Michael, Kennedy, James L., and Sun, Lei

Published
2018

30. Genomics implicates adaptive and innate immunity in Alzheimer’s and Parkinson’s diseases

Author

Gagliano, Sarah A., Pouget, Jennie G., Hardy, John, Knight, Jo, Barnes, Michael R., Ryten, Mina, and Weale, Mike

Abstract

Objectives: We assessed the current genetic evidence for the involvement of various cell types and tissue types in the aetiology of neurodegenerative diseases, especially in relation to the neuroinflammatory hypothesis of neurodegenerative diseases. Methods: We obtained large-scale genome-wide association study (GWAS) summary statistics from Parkinson’s disease (PD), Alzheimer’s disease (AD), and amyotrophic lateral sclerosis (ALS). We used multiple sclerosis (MS), an autoimmune disease of the central nervous system, as a positive control. We applied stratified LD score regression to determine if functional marks for cell type and tissue activity, and gene set lists were enriched for genetic heritability. We compared our results to those from two gene-set enrichment methods (Ingenuity Pathway Analysis and enrichr). Results: There were no significant heritability enrichments for annotations marking genes active within brain regions, but there were for annotations marking genes active within cell-types that form part of both the innate and adaptive immune systems. We found this for MS (as expected) and also for AD and PD. The strongest signals were from the adaptive immune system (e.g. T cells) for PD, and from both the adaptive (e.g. T cells) and innate (e.g. CD14: a marker for monocytes, and CD15: a marker for neutrophils) immune systems for AD. Annotations from the liver were also significant for AD. Pathway analysis provided complementary results. Interpretation: For Alzheimer’s and Parkinson’s disease, we found significant enrichment of heritability in annotations marking gene activity in immune cells.

Published
2016

31. A Comprehensive Analysis of Nuclear-Encoded Mitochondrial Genes in Schizophrenia

Author

Gonçalves, Vanessa F., primary, Cappi, Carolina, additional, Hagen, Christian M., additional, Sequeira, Adolfo, additional, Vawter, Marquis P., additional, Derkach, Andriy, additional, Zai, Clement C., additional, Hedley, Paula L., additional, Bybjerg-Grauholm, Jonas, additional, Pouget, Jennie G., additional, Cuperfain, Ari B., additional, Sullivan, Patrick F., additional, Christiansen, Michael, additional, Kennedy, James L., additional, and Sun, Lei, additional

Published
2018
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33. Cross-disorder analysis of schizophrenia and 19 immune diseases reveals genetic correlation

Author

Pouget, Jennie G, Han, Buhm, Wu, Yang, Mignot, Emmanuel, Ollila, Hanna M, Barker, Jonathan, Spain, Sarah, Dand, Nick, Trembath, Richard, Martin, Javier, Mayes, Maureen D, Bossini-Castillo, Lara, López-Isac, Elena, Jin, Ying, Santorico, Stephanie A, Spritz, Richard A, Raychaudhuri, Soumya, and Knight, Jo

Subjects
Autoimmune disease, 0303 health sciences, education.field_of_study, business.industry, Multiple sclerosis, Population, Genome-wide association study, Human leukocyte antigen, medicine.disease, Genetic correlation, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Primary biliary cirrhosis, Schizophrenia, Immunology, medicine, education, business, 030217 neurology & neurosurgery, 030304 developmental biology
Abstract

Epidemiological studies indicate that many immune diseases occur at different rates among people with schizophrenia compared to the general population. Here, we evaluated whether this phenotypic correlation between immune diseases and schizophrenia might be explained by shared genetic risk factors (genetic correlation). We used data from a large genome-wide association study (GWAS) of schizophrenia (N=35,476 cases and 46,839 controls) to compare the genetic architecture of schizophrenia to 19 immune diseases. First, we evaluated the association with schizophrenia of 581 variants previously reported to be associated with immune diseases at genome-wide significance. We identified three variants with pleiotropic effects, located in regions associated with both schizophrenia and immune disease. Our analyses provided the strongest evidence of pleiotropy at rs1734907 (∼85kb upstream ofEPHB4), a variant which was associated with increased risk of both Crohn’s disease (OR = 1.16, P = 1.67×10−13) and schizophrenia (OR = 1.07, P = 7.55×10−6). Next, we investigated genome-wide sharing of common variants between schizophrenia and immune diseases using polygenic risk scores (PRS) and cross-trait LD Score regression (LDSC). PRS revealed significant genetic overlap with schizophrenia for narcolepsy (p=4.1×10−4), primary biliary cirrhosis (p=1.4×10−8), psoriasis (p=3.6×10−5), systemic lupus erythematosus (p=2.2×10−8), and ulcerative colitis (p=4.3×10−4). Genetic correlations between these immune diseases and schizophrenia, estimated using LDSC, ranged from 0.10 to 0.18 and were consistent with the expected phenotypic correlation based on epidemiological data. We also observed suggestive evidence of sex-dependent genetic correlation between schizophrenia and multiple sclerosis (interaction p=0.02), with genetic risk scores for multiple sclerosis associated with greater risk of schizophrenia among males but not females. Our findings suggest that shared genetic risk factors contribute to the epidemiological co-occurrence of schizophrenia and certain immune diseases, and suggest that in some cases this genetic correlation is sex-dependent.Author SummaryImmune diseases occur at different rates among patients with schizophrenia compared to the general population. While the reasons for this phenotypic correlation are unclear, shared genetic risk (genetic correlation) has been proposed as a contributing factor. Prior studies have estimated the genetic correlation between schizophrenia and a handful of immune diseases, with conflicting results. Here, we performed a comprehensive cross-disorder investigation of schizophrenia and 19 immune diseases. We identified three individual genetic variants associated with both schizophrenia and immune diseases, including a variant nearEPHB4– a gene whose protein product guides the migration of lymphocytes towards infected cells in the immune system and the migration of neuronal axons in the brain. We demonstrated significant genome-wide genetic correlation between schizophrenia and narcolepsy, primary biliary cirrhosis, psoriasis, systemic lupus erythematosus, and ulcerative colitis. Finally, we identified a potential sex-dependent pleiotropic effect between schizophrenia and multiple sclerosis. Our findings point to shared genetic risk for schizophrenia and at least a subset of immune diseases, which likely contributes to their epidemiological co-occurrence. These results raise the possibility that the same genetic variants may exert their effects on neurons or immune cells to influence the development of psychiatric and immune disorders, respectively.

Published
2016
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34. Impact of histamine receptors H1 and H3 polymorphisms on antipsychotic-induced weight gain

Author

Tiwari, Arun K., primary, Zhang, Danning, additional, Pouget, Jennie G., additional, Zai, Clement C., additional, Chowdhury, Nabilah I., additional, Brandl, Eva J., additional, Qin, Li, additional, Freeman, Natalie, additional, Lieberman, Jeffrey A., additional, Meltzer, Herbert Y., additional, Kennedy, James L., additional, and Müller, Daniel J., additional

Published
2016
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35. Rapporteur summaries of plenary, symposia, and oral sessions from the XXIIIrd World Congress of Psychiatric Genetics Meeting in Toronto, Canada, 16–20 October 2015

Author

Zai, Gwyneth, primary, Alberry, Bonnie, additional, Arloth, Janine, additional, Bánlaki, Zsófia, additional, Bares, Cristina, additional, Boot, Erik, additional, Camilo, Caroline, additional, Chadha, Kartikay, additional, Chen, Qi, additional, Cole, Christopher B., additional, Cost, Katherine T., additional, Crow, Megan, additional, Ekpor, Ibene, additional, Fischer, Sascha B., additional, Flatau, Laura, additional, Gagliano, Sarah, additional, Kirli, Umut, additional, Kukshal, Prachi, additional, Labrie, Viviane, additional, Lang, Maren, additional, Lett, Tristram A., additional, Maffioletti, Elisabetta, additional, Maier, Robert, additional, Mihaljevic, Marina, additional, Mittal, Kirti, additional, Monson, Eric T., additional, O’Brien, Niamh L., additional, Østergaard, Søren D., additional, Ovenden, Ellen, additional, Patel, Sejal, additional, Peterson, Roseann E., additional, Pouget, Jennie G., additional, Rovaris, Diego L., additional, Seaman, Lauren, additional, Shankarappa, Bhagya, additional, Tsetsos, Fotis, additional, Vereczkei, Andrea, additional, Wang, Chenyao, additional, Xulu, Khethelo, additional, Yuen, Ryan K.C., additional, Zhao, Jingjing, additional, Zai, Clement C., additional, and Kennedy, James L., additional

Published
2016
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36. A method to decipher pleiotropy by detecting underlying heterogeneity driven by hidden subgroups applied to autoimmune and neuropsychiatric diseases

Author

Han, Buhm, Pouget, Jennie G., Slowikowski, Kamil, Stahl, Eli, Lee, Cue Hyunkyu, Diogo, Dorothee, Hu, Xinli, Park, Yu Rang, Kim, Eunji, Gregersen, Peter K., Dahlqvist, Solbritt Rantapää, Worthington, Jane, Martin, Javier, Eyre, Steve, Klareskog, Lars, Huizinga, Tom, Chen, Wei-Min, Onengut-Gumuscu, Suna, Rich, Stephen S., Wray, Naomi R., Raychaudhuri, Soumya, Han, Buhm, Pouget, Jennie G., Slowikowski, Kamil, Stahl, Eli, Lee, Cue Hyunkyu, Diogo, Dorothee, Hu, Xinli, Park, Yu Rang, Kim, Eunji, Gregersen, Peter K., Dahlqvist, Solbritt Rantapää, Worthington, Jane, Martin, Javier, Eyre, Steve, Klareskog, Lars, Huizinga, Tom, Chen, Wei-Min, Onengut-Gumuscu, Suna, Rich, Stephen S., Wray, Naomi R., and Raychaudhuri, Soumya

Abstract

There is growing evidence of shared risk alleles for complex traits (pleiotropy), including autoimmune and neuropsychiatric diseases. This might be due to sharing among all individuals (whole-group pleiotropy) or a subset of individuals in a genetically heterogeneous cohort (subgroup heterogeneity). Here we describe the use of a well-powered statistic, BUHMBOX, to distinguish between those two situations using genotype data. We observed a shared genetic basis for 11 autoimmune diseases and type 1 diabetes (T1D; P < 1 x 10(-4)) and for 11 autoimmune diseases and rheumatoid arthritis (RA; P < 1 x 10(-3)). This sharing was not explained by subgroup heterogeneity (corrected P-BUHMBOX > 0.2; 6,670 T1D cases and 7,279 RA cases). Genetic sharing between seronegative and seropostive RA (P < 1 x 10(-9)) had significant evidence of subgroup heterogeneity, suggesting a subgroup of seropositive-like cases within seronegative cases (P-BUHMBOX = 0.008; 2,406 seronegative RA cases). We also observed a shared genetic basis for major depressive disorder (MDD) and schizophrenia (P < 1 x 10(-4)) that was not explained by subgroup heterogeneity (P-BUHMBOX = 0.28; 9,238 MDD cases).

Published
2016
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37. Investigating the Causal Relationship of C-Reactive Protein with 32 Complex Somatic and Psychiatric Outcomes : A Large-Scale Cross-Consortium Mendelian Randomization Study

Author

Prins, Bram P., Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E., Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P., Valdes, Ana M., Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D., Tsoi, Lam C., Evangelou, Evangelos, Nair, Rajan P., Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A., Dunstan, Melanie L., Wood, Nicholas W., Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S., Elder, James T., Knight, Jo, Arking, Dan E., Spector, Timothy D., Koeleman, Bobby P C, van Duijn, Cornelia M., Martin, Javier, Morris, Andrew P., Weersma, Rinse K., Wijmenga, Cisca, Munroe, Patricia B., Perry, John R B, Pouget, Jennie G., Jamshidi, Yalda, Snieder, Harold, Alizadeh, Behrooz Z., Prins, Bram P., Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E., Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P., Valdes, Ana M., Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D., Tsoi, Lam C., Evangelou, Evangelos, Nair, Rajan P., Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A., Dunstan, Melanie L., Wood, Nicholas W., Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S., Elder, James T., Knight, Jo, Arking, Dan E., Spector, Timothy D., Koeleman, Bobby P C, van Duijn, Cornelia M., Martin, Javier, Morris, Andrew P., Weersma, Rinse K., Wijmenga, Cisca, Munroe, Patricia B., Perry, John R B, Pouget, Jennie G., Jamshidi, Yalda, Snieder, Harold, and Alizadeh, Behrooz Z.

Published
2016

38. Investigating the causal relationship of C-reactive protein with 32 complex somatic and psychiatric outcomes:a large-scale cross-consortium Mendelian randomization study

Author

Prins, Bram P, Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E, Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P, Valdes, Ana M, Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D, Tsoi, Lam C, Evangelou, Evangelos, Nair, Rajan P, Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A, Dunstan, Melanie L, Wood, Nicholas W, Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S, Elder, James T, Knight, Jo, Arking, Dan E, Spector, Timothy D, Koeleman, Bobby P C, van Duijn, Cornelia M, Martin, Javier, Morris, Andrew P, Weersma, Rinse K, Wijmenga, Cisca, Munroe, Patricia B, Perry, John R B, Pouget, Jennie G, Jamshidi, Yalda, Snieder, Harold, Alizadeh, Behrooz Z, PAGE Consortium, Prins, Bram P, Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E, Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P, Valdes, Ana M, Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D, Tsoi, Lam C, Evangelou, Evangelos, Nair, Rajan P, Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A, Dunstan, Melanie L, Wood, Nicholas W, Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S, Elder, James T, Knight, Jo, Arking, Dan E, Spector, Timothy D, Koeleman, Bobby P C, van Duijn, Cornelia M, Martin, Javier, Morris, Andrew P, Weersma, Rinse K, Wijmenga, Cisca, Munroe, Patricia B, Perry, John R B, Pouget, Jennie G, Jamshidi, Yalda, Snieder, Harold, Alizadeh, Behrooz Z, and PAGE Consortium

Abstract

BACKGROUND: C-reactive protein (CRP) is associated with immune, cardiometabolic, and psychiatric traits and diseases. Yet it is inconclusive whether these associations are causal. METHODS AND FINDINGS: We performed Mendelian randomization (MR) analyses using two genetic risk scores (GRSs) as instrumental variables (IVs). The first GRS consisted of four single nucleotide polymorphisms (SNPs) in the CRP gene (GRSCRP), and the second consisted of 18 SNPs that were significantly associated with CRP levels in the largest genome-wide association study (GWAS) to date (GRSGWAS). To optimize power, we used summary statistics from GWAS consortia and tested the association of these two GRSs with 32 complex somatic and psychiatric outcomes, with up to 123,865 participants per outcome from populations of European ancestry. We performed heterogeneity tests to disentangle the pleiotropic effect of IVs. A Bonferroni-corrected significance level of less than 0.0016 was considered statistically significant. An observed p-value equal to or less than 0.05 was considered nominally significant evidence for a potential causal association, yet to be confirmed. The strengths (F-statistics) of the IVs were 31.92-3,761.29 and 82.32-9,403.21 for GRSCRP and GRSGWAS, respectively. CRP GRSGWAS showed a statistically significant protective relationship of a 10% genetically elevated CRP level with the risk of schizophrenia (odds ratio [OR] 0.86 [95% CI 0.79-0.94]; p < 0.001). We validated this finding with individual-level genotype data from the schizophrenia GWAS (OR 0.96 [95% CI 0.94-0.98]; p < 1.72 × 10-6). Further, we found that a standardized CRP polygenic risk score (CRPPRS) at p-value thresholds of 1 × 10-4, 0.001, 0.01, 0.05, and 0.1 using individual-level data also showed a protective effect (OR < 1.00) against schizophrenia; the first CRPPRS (built of SNPs with p < 1 × 10-4) showed a statistically significant (p < 2.45 × 10-4) protective effect with an OR of 0.97 (95% CI 0.95-0.99). The C

Published
2016

39. Genome-wide association studies suggest limited immune gene enrichment in schizophrenia compared to 5 autoimmune diseases

Author

Pouget, Jennie G., Gonçalves, Vanessa F., Spain, Sarah L., Finucane, Hilary K., Raychaudhuri, Soumya, Kennedy, James L., Knight, Jo, Schizophrenia Working Group of the Psychiatric Genomics Consorti, Pouget, Jennie G., Gonçalves, Vanessa F., Spain, Sarah L., Finucane, Hilary K., Raychaudhuri, Soumya, Kennedy, James L., Knight, Jo, and Schizophrenia Working Group of the Psychiatric Genomics Consorti

Abstract

There has been intense debate over the immunological basis of schizophrenia, and the potential utility of adjunct immunotherapies. The major histocompatibility complex is consistently the most powerful region of association in genome-wide association studies (GWASs) of schizophrenia and has been interpreted as strong genetic evidence supporting the immune hypothesis. However, global pathway analyses provide inconsistent evidence of immune involvement in schizophrenia, and it remains unclear whether genetic data support an immune etiology per se. Here we empirically test the hypothesis that variation in immune genes contributes to schizophrenia. We show that there is no enrichment of immune loci outside of the MHC region in the largest genetic study of schizophrenia conducted to date, in contrast to 5 diseases of known immune origin. Among 108 regions of the genome previously associated with schizophrenia, we identify 6 immune candidates (DPP4, HSPD1, EGR1, CLU, ESAM, NFATC3) encoding proteins with alternative, nonimmune roles in the brain. While our findings do not refute evidence that has accumulated in support of the immune hypothesis, they suggest that genetically mediated alterations in immune function may not play a major role in schizophrenia susceptibility. Instead, there may be a role for pleiotropic effects of a small number of immune genes that also regulate brain development and plasticity. Whether immune alterations drive schizophrenia progression is an important question to be addressed by future research, especially in light of the growing interest in applying immunotherapies in schizophrenia.

Published
2016

40. Investigating the Causal Relationship of C-Reactive Protein with 32 Complex Somatic and Psychiatric Outcomes: A Large-Scale Cross-Consortium Mendelian Randomization Study

Author

Translationele immunologie, Infection & Immunity, Genetica Groep Koeleman, Circulatory Health, Brain, Child Health, Epidemiology & Health Economics, Genetica, Prins, Bram P., Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E., Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P., Valdes, Ana M., Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D., Tsoi, Lam C., Evangelou, Evangelos, Nair, Rajan P., Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A., Dunstan, Melanie L., Wood, Nicholas W., Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S., Elder, James T., Knight, Jo, Arking, Dan E., Spector, Timothy D., Koeleman, Bobby P C, van Duijn, Cornelia M., Martin, Javier, Morris, Andrew P., Weersma, Rinse K., Wijmenga, Cisca, Munroe, Patricia B., Perry, John R B, Pouget, Jennie G., Jamshidi, Yalda, Snieder, Harold, Alizadeh, Behrooz Z., Translationele immunologie, Infection & Immunity, Genetica Groep Koeleman, Circulatory Health, Brain, Child Health, Epidemiology & Health Economics, Genetica, Prins, Bram P., Abbasi, Ali, Wong, Anson, Vaez, Ahmad, Nolte, Ilja, Franceschini, Nora, Stuart, Philip E., Guterriez Achury, Javier, Mistry, Vanisha, Bradfield, Jonathan P., Valdes, Ana M., Bras, Jose, Shatunov, Aleksey, Lu, Chen, Han, Buhm, Raychaudhuri, Soumya, Bevan, Steve, Mayes, Maureen D., Tsoi, Lam C., Evangelou, Evangelos, Nair, Rajan P., Grant, Struan F A, Polychronakos, Constantin, Radstake, Timothy R D, van Heel, David A., Dunstan, Melanie L., Wood, Nicholas W., Al-Chalabi, Ammar, Dehghan, Abbas, Hakonarson, Hakon, Markus, Hugh S., Elder, James T., Knight, Jo, Arking, Dan E., Spector, Timothy D., Koeleman, Bobby P C, van Duijn, Cornelia M., Martin, Javier, Morris, Andrew P., Weersma, Rinse K., Wijmenga, Cisca, Munroe, Patricia B., Perry, John R B, Pouget, Jennie G., Jamshidi, Yalda, Snieder, Harold, and Alizadeh, Behrooz Z.

Published
2016

43. Investigation of TSPO variants in schizophrenia and antipsychotic treatment outcomes

Author

Pouget, Jennie G., Gonçalves, Vanessa F., Nurmi, Erika L., Laughlin, Christopher P., Mallya, Karyn S., McCracken, James T., Aman, Michael G., McDougle, Christopher J., Scahill, Lawrence, Misener, Virginia L., Tiwari, Arun K., Zai, Clement C., Brandl, Eva J., Felsky, Daniel, Leung, Amy Q., Lieberman, Jeffrey A., Meltzer, Herbert Y., Potkin, Steven G., Niedling, Charlotte, Steimer, Werner, Leucht, Stefan, Knight, Jo, Müller, Daniel J., Kennedy, James L., Pouget, Jennie G., Gonçalves, Vanessa F., Nurmi, Erika L., Laughlin, Christopher P., Mallya, Karyn S., McCracken, James T., Aman, Michael G., McDougle, Christopher J., Scahill, Lawrence, Misener, Virginia L., Tiwari, Arun K., Zai, Clement C., Brandl, Eva J., Felsky, Daniel, Leung, Amy Q., Lieberman, Jeffrey A., Meltzer, Herbert Y., Potkin, Steven G., Niedling, Charlotte, Steimer, Werner, Leucht, Stefan, Knight, Jo, Müller, Daniel J., and Kennedy, James L.

Abstract

AIM: TSPO is a neuroinflammatory biomarker and emerging therapeutic target in psychiatric disorders. We evaluated whether TSPO polymorphisms contribute to interindividual variability in schizophrenia, antipsychotic efficacy and antipsychotic-induced weight gain. PATIENTS & METHODS: We analyzed TSPO polymorphisms in 670 schizophrenia cases and 775 healthy controls. Gene-gene interactions between TSPO and other mitochondrial membrane protein-encoding genes (VDAC1 and ANT1) were explored. Positive findings were evaluated in two independent samples (Munich, n = 300; RUPP, n = 119). RESULTS: TSPO rs6971 was independently associated with antipsychotic-induced weight gain in the discovery (puncor = 0.04) and RUPP samples (p = 3.00 × 10(-3)), and interacted with ANT1 rs10024068 in the discovery (p = 1.15 × 10(-3)) and RUPP samples (p = 2.76 × 10(-4)). CONCLUSION: Our findings highlight TSPO as a candidate for future investigations of antipsychotic-induced weight gain, and support the involvement of mitochondrial membrane components in this serious treatment side effect.

Published
2015

45. Impact of histamine receptors H1 and H3 polymorphisms on antipsychotic-induced weight gain.

Author

Tiwari, Arun K., Zhang, Danning, Pouget, Jennie G., Zai, Clement C., Chowdhury, Nabilah I., Brandl, Eva J., Qin, Li, Freeman, Natalie, Lieberman, Jeffrey A., Meltzer, Herbert Y., Kennedy, James L., and Müller, Daniel J.

Subjects
ANTIPSYCHOTIC agents, SCHIZOPHRENIA, PATHOLOGICAL psychology, PEOPLE with schizophrenia, OLANZAPINE
Abstract

Objectives: A positive correlation between antipsychotic-induced weight gain (AIWG) and the antagonist effect of antipsychotic drugs at the histamine H1 receptor (HRH1) as well as the agonist effect at the histamine H3 receptor (HRH3) in the brain has been consistently demonstrated. We investigated the potential impact of single-nucleotide polymorphisms (SNPs) in HRH1 and HRH3 genes on AIWG. Methods: We analysed 40 tagSNPs in HRH1 (n = 34) and HRH3 (n = 6) in schizophrenia/schizoaffective disorder patients (n = 193) primarily treated with clozapine or olanzapine for up to 14 weeks. Linear regression was used to evaluate the association between SNPs and AIWG, with baseline weight and treatment duration as covariates. Results: In HRH1, a nominal association of rs7639145 with AIWG was observed in patients of European ancestry treated with either clozapine or olanzapine (P= 0.043; β = 1.658; n = 77). We observed nominal association for two HRH1 SNPs rs346074 (P = 0.002; β = -5.024) and rs13064530 (P= 0.004; β = -5.158) in patients of African ancestry treated with either clozapine or olanzapine (n = 37). However, the above associations are not significant after correcting for multiple testing. In HRH3, we did not observe association in either ancestry. Conclusions: The current study suggests that SNPs in HRH1 and HRH3 may not have a major role in AIWG. [ABSTRACT FROM AUTHOR]

Published
2018
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47. The three-year incidence of fracture in chronic kidney disease

Author

Naylor, Kyla L., primary, McArthur, Eric, additional, Leslie, William D., additional, Fraser, Lisa-Ann, additional, Jamal, Sophie A., additional, Cadarette, Suzanne M., additional, Pouget, Jennie G., additional, Lok, Charmaine E., additional, Hodsman, Anthony B., additional, Adachi, Jonathan D., additional, and Garg, Amit X., additional

Published
2014
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50. Increased Nigral SLC6A3 Activity in Schizophrenia Patients: Findings From the Toronto-McLean Cohorts.

Author

Kennedy, James L., Nian Xiong, Jinlong Yu, Zai, Clement C., Pouget, Jennie G., Jie Li, Kefu Liu, Hong Qing, Tao Wang, Martin, Eden, Levy, Deborah L., and Zhicheng Lin

Subjects
GENETICS of schizophrenia, ANALYSIS of variance, BIOMARKERS, BRAIN, DOPAMINE, POLYMERASE chain reaction, RESEARCH funding, SMOKING, T-test (Statistics), PHENOTYPES, COMORBIDITY
Published
2016
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