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3. DNA-methylation and immunological response in medication overuse headache

Author

Carlsen, Louise Ninett, Hansen, Christine Søholm, Kogelman, Lisette J.A., Werge, Thomas Mears, Ullum, Henrik, Bybjerg-Grauholm, Jonas, Hansen, Thomas Folkmann, Jensen, Rigmor Højland, Carlsen, Louise Ninett, Hansen, Christine Søholm, Kogelman, Lisette J.A., Werge, Thomas Mears, Ullum, Henrik, Bybjerg-Grauholm, Jonas, Hansen, Thomas Folkmann, and Jensen, Rigmor Højland

Abstract

OBJECTIVE: To investigate whether medication-overuse headache patients have differential DNA-methylation pattern. METHODS: We collected blood samples from 120 medication-overuse headache-patients, 57 controls (29 episodic migraine patients and 28 healthy controls) in a hypothesis-generating cross-sectional case-control pilot study; 100 of the medication-overuse headache-patients were followed for six months and samples were collected at two and six months for the longitudinal methylation analyses. Blood cell proportions of leucocytes (neutrophils, NK-cells, monocytes, CD8+ and CD4+ T-cells, and B-cells) and the neutrophile-lymphocyte ratio were estimated using methylation data as a measure for immunological analysis and a cell type-specific epigenome wide association study was conducted between medication-overuse headache-patients and controls, and longitudinally for reduction in headache days/month among medication-overuse headache-patients. RESULTS: We found a higher neutrophile-lymphocyte ratio in medication-overuse headache-patients compared to controls, indicating a higher immunological response in medication-overuse headache-patients (false discovery rate (adjusted p-value)<0.001). Reduction in headache days/month (9.8; 95% CI 8.1-11.5) was associated with lower neutrophile-lymphocyte ratio (false discovery rate adjusted p-value = 0.041).Three genes (CORIN, CCKBR and CLDN9) were hypermethylated in specific cell types in medication-overuse headache-patients compared to controls. No methylation differences were associated with reduction in headache days in medication-overuse headache-patients after six months. CONCLUSION: This pilot study was consistent with higher immunological response in medication-overuse headache-patients which decreased with a reduction in headache days in longitudinal analysis. medication-overuse headache-patients exhibited differential methylation in innate immune cells but did not exhibit longitudinal differences with alterations

Published
2023

4. sj-pdf-2-cep-10.1177_03331024221147482 - Supplemental material for DNA-methylation and immunological response in medication overuse headache

Author

Carlsen, Louise Ninett, Hansen, Christine Søholm, Kogelman, Lisette J. A., Werge, Thomas Mears, Ullum, Henrik, Bybjerg-Grauholm, Jonas, Hansen, Thomas Folkmann, and Jensen, Rigmor Højland

Subjects
FOS: Psychology, FOS: Clinical medicine, 170199 Psychology not elsewhere classified, 110319 Psychiatry (incl. Psychotherapy), 110306 Endocrinology, 111599 Pharmacology and Pharmaceutical Sciences not elsewhere classified, 110904 Neurology and Neuromuscular Diseases, Neuroscience
Abstract

Supplemental material, sj-pdf-2-cep-10.1177_03331024221147482 for DNA-methylation and immunological response in medication overuse headache by Louise Ninett Carlsen, Christine Søholm Hansen, Lisette J. A. Kogelman, Thomas Mears Werge, Henrik Ullum, Jonas Bybjerg-Grauholm, Thomas Folkmann Hansen and Rigmor Højland Jensen in Cephalalgia

Published
2023
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6. Additional file 1 of Co-occurring hydrocephalus in autism spectrum disorder: a Danish population-based cohort study

Author

Munch, Tina Nørgaard, Hedley, Paula Louise, Hagen, Christian Munch, Bækvad-Hansen, Marie, Bybjerg-Grauholm, Jonas, Grove, Jakob, Nordentoft, Merete, Børglum, Anders Dupont, Mortensen, Preben Bo, Werge, Thomas Mears, Melbye, Mads, Hougaard, David Michael, and Christiansen, Michael

Subjects
mental disorders, behavioral disciplines and activities, nervous system diseases
Abstract

Additional file 1: Figure S1. Permutation tests of association between hydrocephalus and autism spectrum disorder. Figure S2. Interval between first-time diagnosis of ASD and first-time diagnosis of hydrocephalus (HC) in all cases (n = 68) of ASD and HC and in all cases of childhood autism (n = 23) and HC. Table S1. Age at diagnosis and gender distribution of the hydrocephalus patients by psychiatric co-diagnosis.

Published
2021
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7. Co-occurring hydrocephalus in autism spectrum disorder:a Danish population-based cohort study

Author

Munch, Tina Nørgaard, Hedley, Paula Louise, Hagen, Christian Munch, Bækvad-Hansen, Marie, Bybjerg-Grauholm, Jonas, Grove, Jakob, Nordentoft, Merete, Børglum, Anders Dupont, Mortensen, Preben Bo, Werge, Thomas Mears, Melbye, Mads, Hougaard, David Michael, Christiansen, Michael, Munch, Tina Nørgaard, Hedley, Paula Louise, Hagen, Christian Munch, Bækvad-Hansen, Marie, Bybjerg-Grauholm, Jonas, Grove, Jakob, Nordentoft, Merete, Børglum, Anders Dupont, Mortensen, Preben Bo, Werge, Thomas Mears, Melbye, Mads, Hougaard, David Michael, and Christiansen, Michael

Abstract

Background: The association between autism spectrum disorder and hydrocephalus is not well understood, despite demonstrated links between autism spectrum disorder and cerebrospinal fluid abnormalities. Based on the hypothesis that autism spectrum disorder and hydrocephalus may, at least in some cases, be two manifestations of a shared congenital brain pathology, we investigated the potential association between autism spectrum disorder and hydrocephalus in a large Danish population-based cohort. Methods: Patients and controls were obtained from the Lundbeck Foundation Initiative for Integrative Psychiatric Research iPSYCH2012 case-cohort, which includes all patients with selected psychiatric disorders born in Denmark 1981–2005 along with randomly selected population controls (end of follow-up, December 31, 2016). The associations between individual psychiatric disorders and hydrocephalus were estimated using binary logistic regression with adjustment for age and sex. Results: The cohort consisted of 86,571 individuals, of which 14,654 were diagnosed with autism spectrum disorder, 28,606 were population controls, and the remaining were diagnosed with other psychiatric disorders. We identified 201 hydrocephalus cases; 68 among autism spectrum disorder patients and 40 among controls (OR 3.77, 95% CI 2.48–5.78), which corresponds to an absolute risk of 0.46 % (i.e. approximately one in 217 children with autism spectrum disorder had co-occurring hydrocephalus). The autism spectrum disorder-hydrocephalus association was significant over the entire subgroup spectrum of autism spectrum disorder. Conclusions: Given the considerable risk of hydrocephalus among patients with autism spectrum disorder, we suggest that patients with autism spectrum disorder should be evaluated for co-occurring hydrocephalus on a routine basis as timely neurosurgical intervention is important. Likewise, attention must be paid to traits of autism spectrum disorder in children with hydrocephalus.

Published
2021

8. Co-occurring hydrocephalus in autism spectrum disorder: a Danish population-based cohort study

Author

Munch, Tina Nørgaard, primary, Hedley, Paula Louise, additional, Hagen, Christian Munch, additional, Bækvad-Hansen, Marie, additional, Bybjerg-Grauholm, Jonas, additional, Grove, Jakob, additional, Nordentoft, Merete, additional, Børglum, Anders Dupont, additional, Mortensen, Preben Bo, additional, Werge, Thomas Mears, additional, Melbye, Mads, additional, Hougaard, David Michael, additional, and Christiansen, Michael, additional

Published
2021
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9. Elevated DNA Methylation Gestational Age is Associated with the Risk of Later Bipolar Disorder and Anorexia Nervosa in Twins

Author

Søholm Hansen, Christine, primary, Starnawska, Anna, additional, Drong, Alexander Werner, additional, Weinsheimer, Shantel Marie, additional, Bækvad-Hansen, Marie, additional, Helenius, Dorte, additional, Giørtz Pedersen, Marianne, additional, Bøcker Pedersen, Carsten, additional, Mortensen, Preben Bo, additional, Christiansen, Michael, additional, Hougaard, David Michael, additional, Lindgren, Cecilia, additional, Werge, Thomas Mears, additional, Bybjerg-Grauholm, Jonas, additional, and Demur, Alfonso Buil, additional

Published
2020
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10. Individuals with 22q11.2 deletion syndrome show intact prediction but reduced adaptation in responses to repeated sounds:Evidence from Bayesian mapping

Author

Larsen, Kit Melissa, Mørup, Morten, Birknow, Michelle Rosgaard, Fischer, Elvira, Olsen, Line, Didriksen, Michael, Baaré, William Frans Christiaan, Werge, Thomas Mears, Garrido, Marta Isabel, Siebner, Hartwig Roman, Larsen, Kit Melissa, Mørup, Morten, Birknow, Michelle Rosgaard, Fischer, Elvira, Olsen, Line, Didriksen, Michael, Baaré, William Frans Christiaan, Werge, Thomas Mears, Garrido, Marta Isabel, and Siebner, Hartwig Roman

Abstract

One of the most common copy number variants, the 22q11.2 microdeletion, confers an increased risk for schizophrenia. Since schizophrenia has been associated with an aberrant neural response to repeated stimuli through both reduced adaptation and prediction, we here hypothesized that this may also be the case in nonpsychotic individuals with a 22q11.2 deletion. We recorded high-density EEG from 19 individuals with 22q11.2 deletion syndrome (12–25 years), as well as 27 healthy volunteers with comparable age and sex distribution, while they listened to a sequence of sounds arranged in a roving oddball paradigm. Using posterior probability maps and dynamic causal modelling we tested three different models accounting for repetition dependent changes in cortical responses as well as in effective connectivity; namely an adaptation model, a prediction model, and a model including both adaptation and prediction. Repetition-dependent changes were parametrically modulated by a combination of adaptation and prediction and were apparent in both cortical responses and in the underlying effective connectivity. This effect was reduced in individuals with a 22q11.2 deletion and was negatively correlated with negative symptom severity. Follow-up analysis showed that the reduced effect of the combined adaptation and prediction model seen in individuals with 22q11.2 deletion was driven by reduced adaptation rather than prediction failure. Our findings suggest that adaptation is reduced in individuals with a 22q11.2 deletion, which can be interpreted in light of the framework of predictive coding as a failure to suppress prediction errors.

Published
2019

11. Individuals with 22q11.2 deletion syndrome show intact prediction but reduced adaptation in responses to repeated sounds: evidence from Bayesian mapping

Author

Larsen, Kit Melissa, primary, Mørup, Morten, additional, Birknow, Michelle Rosgaard, additional, Fischer, Elvira, additional, Olsen, Line, additional, Didriksen, Michael, additional, Christiaan Baaré, William Frans, additional, Werge, Thomas Mears, additional, Garrido, Marta Isabel, additional, and Siebner, Hartwig Roman, additional

Published
2018
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12. High-Quality Exome Sequencing of Whole-Genome Amplified Neonatal Dried Blood Spot DNA

Author

Poulsen, Jesper Buchhave, Lescai, Francesco, Grove, Jakob, Bækvad-Hansen, Marie, Christiansen, Michael, Hagen, Christian Munch, Maller, Julian, Stevens, Christine, Li, Shenting, Li, Qibin, Sun, Jihua, Wang, Jun, Nordentoft, Merete, Werge, Thomas Mears, Mortensen, Preben Bo, Børglum, Anders Dupont, Daly, Mark, Hougaard, David Michael, Bybjerg-Grauholm, Jonas, Hollegaard, Mads Vilhelm, Poulsen, Jesper Buchhave, Lescai, Francesco, Grove, Jakob, Bækvad-Hansen, Marie, Christiansen, Michael, Hagen, Christian Munch, Maller, Julian, Stevens, Christine, Li, Shenting, Li, Qibin, Sun, Jihua, Wang, Jun, Nordentoft, Merete, Werge, Thomas Mears, Mortensen, Preben Bo, Børglum, Anders Dupont, Daly, Mark, Hougaard, David Michael, Bybjerg-Grauholm, Jonas, and Hollegaard, Mads Vilhelm

Abstract

Stored neonatal dried blood spot (DBS) samples from neonatal screening programmes are a valuable diagnostic and research resource. Combined with information from national health registries they can be used in population-based studies of genetic diseases. DNA extracted from neonatal DBSs can be amplified to obtain micrograms of an otherwise limited resource, referred to as whole-genome amplified DNA (wgaDNA). Here we investigate the robustness of exome sequencing of wgaDNA of neonatal DBS samples. We conducted three pilot studies of seven, eight and seven subjects, respectively. For each subject we analysed a neonatal DBS sample and corresponding adult whole-blood (WB) reference sample. Different DNA sample types were prepared for each of the subjects. Pilot 1: wgaDNA of 2x3.2mm neonatal DBSs (DBS_2x3.2) and raw DNA extract of the WB reference sample (WB_ref). Pilot 2: DBS_2x3.2, WB_ref and a WB_ref replica sharing DNA extract with the WB_ref sample. Pilot 3: DBS_2x3.2, WB_ref, wgaDNA of 2x1.6 mm neonatal DBSs and wgaDNA of the WB reference sample. Following sequencing and data analysis, we compared pairwise variant calls to obtain a measure of similarity--the concordance rate. Concordance rates were slightly lower when comparing DBS vs WB sample types than for any two WB sample types of the same subject before filtering of the variant calls. The overall concordance rates were dependent on the variant type, with SNPs performing best. Post-filtering, the comparisons of DBS vs WB and WB vs WB sample types yielded similar concordance rates, with values close to 100%. WgaDNA of neonatal DBS samples performs with great accuracy and efficiency in exome sequencing. The wgaDNA performed similarly to matched high-quality reference--whole-blood DNA--based on concordance rates calculated from variant calls. No differences were observed substituting 2x3.2 with 2x1.6 mm discs, allowing for additional reduction of sample material in future projects.

Published
2016

13. High-Quality Exome Sequencing of Whole-Genome Amplified Neonatal Dried Blood Spot DNA

Author

Poulsen, Jesper Buchhave, primary, Lescai, Francesco, additional, Grove, Jakob, additional, Bækvad-Hansen, Marie, additional, Christiansen, Michael, additional, Hagen, Christian Munch, additional, Maller, Julian, additional, Stevens, Christine, additional, Li, Shenting, additional, Li, Qibin, additional, Sun, Jihua, additional, Wang, Jun, additional, Nordentoft, Merete, additional, Werge, Thomas Mears, additional, Mortensen, Preben Bo, additional, Børglum, Anders Dupont, additional, Daly, Mark, additional, Hougaard, David Michael, additional, Bybjerg-Grauholm, Jonas, additional, and Hollegaard, Mads Vilhelm, additional

Published
2016
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14. Den genetiske hjerne

Author

Tommerup, Niels, Christensen, K@åre, Werge, Thomas Mears, Tommerup, Niels, Christensen, K@åre, and Werge, Thomas Mears

Published
2013

15. Genome-wide significant associations in schizophrenia to ITIH3/4, CACNA1C and SDCCAG8, and extensive replication of associations reported by the Schizophrenia PGC

Author

Hamshere, M L, Walters, J T R, Smith, R, Richards, Alan, Green, E, Grozeva, D, Jones, Ian, Forty, L, Jones, Leigh Robert, Gordon-Smith, K, Riley, B, O'Neill, T, Kendler, K S, Sklar, P, Purcell, S, Kranz, J, Morris, David Jackson, Gill, M, Holmans, P, Craddock, N, Corvin, A, Owen, M J, O'Donovan, M C, Hansen, Thomas, Olsen, Line, Ingason, Andrés, Schmock, Henriette, Skjødt, Celina, Rosengren, Anders, Høffding, Louise.K.Enggaard, Thygesen, Johan Hilge, Werge, Thomas Mears, Hamshere, M L, Walters, J T R, Smith, R, Richards, Alan, Green, E, Grozeva, D, Jones, Ian, Forty, L, Jones, Leigh Robert, Gordon-Smith, K, Riley, B, O'Neill, T, Kendler, K S, Sklar, P, Purcell, S, Kranz, J, Morris, David Jackson, Gill, M, Holmans, P, Craddock, N, Corvin, A, Owen, M J, O'Donovan, M C, Hansen, Thomas, Olsen, Line, Ingason, Andrés, Schmock, Henriette, Skjødt, Celina, Rosengren, Anders, Høffding, Louise.K.Enggaard, Thygesen, Johan Hilge, and Werge, Thomas Mears

Abstract

The Schizophrenia Psychiatric Genome-Wide Association Study Consortium (PGC) highlighted 81 single-nucleotide polymorphisms (SNPs) with moderate evidence for association to schizophrenia. After follow-up in independent samples, seven loci attained genome-wide significance (GWS), but multi-locus tests suggested some SNPs that did not do so represented true associations. We tested 78 of the 81 SNPs in 2640 individuals with a clinical diagnosis of schizophrenia attending a clozapine clinic (CLOZUK), 2504 cases with a research diagnosis of bipolar disorder, and 2878 controls. In CLOZUK, we obtained significant replication to the PGC-associated allele for no fewer than 37 (47%) of the SNPs, including many prior GWS major histocompatibility complex (MHC) SNPs as well as 3/6 non-MHC SNPs for which we had data that were reported as GWS by the PGC. After combining the new schizophrenia data with those of the PGC, variants at three loci (ITIH3/4, CACNA1C and SDCCAG8) that had not previously been GWS in schizophrenia attained that level of support. In bipolar disorder, we also obtained significant evidence for association for 21% of the alleles that had been associated with schizophrenia in the PGC. Our study independently confirms association to three loci previously reported to be GWS in schizophrenia, and identifies the first GWS evidence in schizophrenia for a further three loci. Given the number of independent replications and the power of our sample, we estimate 98% (confidence interval (CI) 78-100%) of the original set of 78 SNPs represent true associations. We also provide strong evidence for overlap in genetic risk between schizophrenia and bipolar disorder.Molecular Psychiatry advance online publication, 22 May 2012; doi:10.1038/mp.2012.67.

Published
2013

16. Schizophrenia genetic variants are not associated with intelligence

Author

van Scheltinga, A F Terwisscha, Bakker, S C, van Haren, N E M, Derks, E M, Buizer-Voskamp, J E, Cahn, W, Ripke, S, Ophoff, R A, Kahn, R S, Werge, Thomas Mears, Hansen, Thomas, Ingason, Andrés, van Scheltinga, A F Terwisscha, Bakker, S C, van Haren, N E M, Derks, E M, Buizer-Voskamp, J E, Cahn, W, Ripke, S, Ophoff, R A, Kahn, R S, Werge, Thomas Mears, Hansen, Thomas, and Ingason, Andrés

Abstract

BACKGROUND: Schizophrenia is associated with lower pre-morbid intelligence (IQ) in addition to (pre-morbid) cognitive decline. Both schizophrenia and IQ are highly heritable traits. Therefore, we hypothesized that genetic variants associated with schizophrenia, including copy number variants (CNVs) and a polygenic schizophrenia (risk) score (PSS), may influence intelligence. Method IQ was estimated with the Wechsler Adult Intelligence Scale (WAIS). CNVs were determined from single nucleotide polymorphism (SNP) data using the QuantiSNP and PennCNV algorithms. For the PSS, odds ratios for genome-wide SNP data were calculated in a sample collected by the Psychiatric Genome-Wide Association Study (GWAS) Consortium (8690 schizophrenia patients and 11 831 controls). These were used to calculate individual PSSs in our independent sample of 350 schizophrenia patients and 322 healthy controls. RESULTS: Although significantly more genes were disrupted by deletions in schizophrenia patients compared to controls (p = 0.009), there was no effect of CNV measures on IQ. The PSS was associated with disease status (R 2 = 0.055, p = 2.1 × 10-7) and with IQ in the entire sample (R 2 = 0.018, p = 0.0008) but the effect on IQ disappeared after correction for disease status. CONCLUSIONS: Our data suggest that rare and common schizophrenia-associated variants do not explain the variation in IQ in healthy subjects or in schizophrenia patients. Thus, reductions in IQ in schizophrenia patients may be secondary to other processes related to schizophrenia risk.

Published
2013

17. Genetic Schizophrenia Risk Variants Jointly Modulate Total Brain and White Matter Volume

Author

Terwisscha van Scheltinga, Afke F, Bakker, Steven C, van Haren, Neeltje E M, Derks, Eske M, Buizer-Voskamp, Jacobine E, Boos, Heleen B M, Cahn, Wiepke, Hulshoff Pol, Hilleke E, Ripke, Stephan, Ophoff, Roel A, Kahn, René S, Jakobsen, Klaus Damgaard, Hansen, Thomas, Ingason, Andrés, Duong, Linh, Rasmussen, Henrik Berg, Olsen, Line, Nordentoft, Merete, Jürgens, Gesche, Glenthøj, Birte Yding, Wang, August Gabriel, Werge, Thomas Mears, Terwisscha van Scheltinga, Afke F, Bakker, Steven C, van Haren, Neeltje E M, Derks, Eske M, Buizer-Voskamp, Jacobine E, Boos, Heleen B M, Cahn, Wiepke, Hulshoff Pol, Hilleke E, Ripke, Stephan, Ophoff, Roel A, Kahn, René S, Jakobsen, Klaus Damgaard, Hansen, Thomas, Ingason, Andrés, Duong, Linh, Rasmussen, Henrik Berg, Olsen, Line, Nordentoft, Merete, Jürgens, Gesche, Glenthøj, Birte Yding, Wang, August Gabriel, and Werge, Thomas Mears

Abstract

BACKGROUND: Thousands of common single nucleotide polymorphisms (SNPs) are weakly associated with schizophrenia. It is likely that subsets of disease-associated SNPs are associated with distinct heritable disease-associated phenotypes. Therefore, we examined the shared genetic susceptibility modulating schizophrenia and brain volume. METHODS: Odds ratios for genome-wide SNP data were calculated in the sample collected by the Psychiatric Genome-wide Association Study Consortium (8690 schizophrenia patients and 11,831 control subjects, excluding subjects from the present study). These were used to calculate individual polygenic schizophrenia (risk) scores in an independent sample of 152 schizophrenia patients and 142 healthy control subjects with available structural magnetic resonance imaging scans. RESULTS: In the entire group, the polygenic schizophrenia score was significantly associated with total brain volume (R(2)=.048, p=1.6×10(-4)) and white matter volume (R(2)=.051, p=8.6×10(-5)) equally in patients and control subjects. The number of (independent) SNPs that substantially influenced both disease risk and white matter (n=2020) was much smaller than the entire set of SNPs that modulated disease status (n=14,751). From the set of 2020 SNPs, a group of 186 SNPs showed most evidence for association with white matter volume and an explorative functional analysis showed that these SNPs were located in genes with neuronal functions. CONCLUSIONS: These results indicate that a relatively small subset of schizophrenia genetic risk variants is related to the (normal) development of white matter. This, in turn, suggests that disruptions in white matter growth increase the susceptibility to develop schizophrenia.

Published
2013

18. Genome-wide association study of multiplex schizophrenia pedigrees

Author

Levinson, Douglas F, Shi, Jianxin, Wang, Kai, Oh, Sang, Riley, Brien, Pulver, Ann E, Wildenauer, Dieter B, Laurent, Claudine, Mowry, Bryan J, Gejman, Pablo V, Owen, Michael J, Kendler, Kenneth S, Nestadt, Gerald, Schwab, Sibylle G, Mallet, Jacques, Nertney, Deborah, Sanders, Alan R, Williams, Nigel M, Wormley, Brandon, Lasseter, Virginia K, Albus, Margot, Godard-Bauché, Stephanie, Alexander, Madeline, Duan, Jubao, O'Donovan, Michael C, Walsh, Dermot, O'Neill, Anthony, Papadimitriou, George N, Dikeos, Dimitris, Maier, Wolfgang, Lerer, Bernard, Campion, Dominique, Cohen, David, Jay, Maurice, Fanous, Ayman, Eichhammer, Peter, Silverman, Jeremy M, Norton, Nadine, Zhang, Nancy, Hakonarson, Hakon, Gao, Cynthia, Citri, Ami, Hansen, Mark, Ripke, Stephan, Dudbridge, Frank, Holmans, Peter A, Werge, Thomas Mears, Levinson, Douglas F, Shi, Jianxin, Wang, Kai, Oh, Sang, Riley, Brien, Pulver, Ann E, Wildenauer, Dieter B, Laurent, Claudine, Mowry, Bryan J, Gejman, Pablo V, Owen, Michael J, Kendler, Kenneth S, Nestadt, Gerald, Schwab, Sibylle G, Mallet, Jacques, Nertney, Deborah, Sanders, Alan R, Williams, Nigel M, Wormley, Brandon, Lasseter, Virginia K, Albus, Margot, Godard-Bauché, Stephanie, Alexander, Madeline, Duan, Jubao, O'Donovan, Michael C, Walsh, Dermot, O'Neill, Anthony, Papadimitriou, George N, Dikeos, Dimitris, Maier, Wolfgang, Lerer, Bernard, Campion, Dominique, Cohen, David, Jay, Maurice, Fanous, Ayman, Eichhammer, Peter, Silverman, Jeremy M, Norton, Nadine, Zhang, Nancy, Hakonarson, Hakon, Gao, Cynthia, Citri, Ami, Hansen, Mark, Ripke, Stephan, Dudbridge, Frank, Holmans, Peter A, and Werge, Thomas Mears

Abstract

The authors used a genome-wide association study (GWAS) of multiply affected families to investigate the association of schizophrenia to common single-nucleotide polymorphisms (SNPs) and rare copy number variants (CNVs).

Published
2012

19. Expression QTL analysis of top loci from GWAS meta-analysis highlights additional schizophrenia candidate genes

Author

de Jong, Simone, van Eijk, Kristel R, Zeegers, Dave W L H, Strengman, Eric, Janson, Esther, Veldink, Jan H, van den Berg, Leonard H, Cahn, Wiepke, Kahn, René S, Boks, Marco P M, Ophoff, Roel A, Werge, Thomas Mears, Hansen, Thomas, Ingason, Andrés, Olsen, Line, Thygesen, Johan Hilge, de Jong, Simone, van Eijk, Kristel R, Zeegers, Dave W L H, Strengman, Eric, Janson, Esther, Veldink, Jan H, van den Berg, Leonard H, Cahn, Wiepke, Kahn, René S, Boks, Marco P M, Ophoff, Roel A, Werge, Thomas Mears, Hansen, Thomas, Ingason, Andrés, Olsen, Line, and Thygesen, Johan Hilge

Abstract

There is genetic evidence that schizophrenia is a polygenic disorder with a large number of loci of small effect on disease susceptibility. Genome-wide association studies (GWASs) of schizophrenia have had limited success, with the best finding at the MHC locus at chromosome 6p. A recent effort of the Psychiatric GWAS consortium (PGC) yielded five novel loci for schizophrenia. In this study, we aim to highlight additional schizophrenia susceptibility loci from the PGC study by combining the top association findings from the discovery stage (9394 schizophrenia cases and 12 462 controls) with expression QTLs (eQTLs) and differential gene expression in whole blood of schizophrenia patients and controls. We examined the 6192 single-nucleotide polymorphisms (SNPs) with significance threshold at P

Published
2012

20. Estimating the proportion of variation in susceptibility to schizophrenia captured by common SNPs

Author

Lee, S Hong, DeCandia, Teresa R, Ripke, Stephan, Yang, Jian, Sullivan, Patrick F, Goddard, Michael E, Keller, Matthew C, Visscher, Peter M, Wray, Naomi R, Hansen, Thomas Folkmann, Ingason, Andrés, Olsen, Line, Rasmussen, Henrik Berg, Werge, Thomas Mears, Lee, S Hong, DeCandia, Teresa R, Ripke, Stephan, Yang, Jian, Sullivan, Patrick F, Goddard, Michael E, Keller, Matthew C, Visscher, Peter M, Wray, Naomi R, Hansen, Thomas Folkmann, Ingason, Andrés, Olsen, Line, Rasmussen, Henrik Berg, and Werge, Thomas Mears

Abstract

Schizophrenia is a complex disorder caused by both genetic and environmental factors. Using 9,087 affected individuals, 12,171 controls and 915,354 imputed SNPs from the Schizophrenia Psychiatric Genome-Wide Association Study (GWAS) Consortium (PGC-SCZ), we estimate that 23% (s.e. = 1%) of variation in liability to schizophrenia is captured by SNPs. We show that a substantial proportion of this variation must be the result of common causal variants, that the variance explained by each chromosome is linearly related to its length (r = 0.89, P = 2.6 × 10(-8)), that the genetic basis of schizophrenia is the same in males and females, and that a disproportionate proportion of variation is attributable to a set of 2,725 genes expressed in the central nervous system (CNS; P = 7.6 × 10(-8)). These results are consistent with a polygenic genetic architecture and imply more individual SNP associations will be detected for this disease as sample size increases.

Published
2012

21. Investigation of the genetic association between quantitative measures of psychosis and schizophrenia:a polygenic risk score analysis

Author

Derks, Eske M, Vorstman, Jacob A S, Ripke, Stephan, Kahn, Rene S, Ophoff, Roel A, Hansen, Thomas, Olsen, Line, Jakobsen, Klaus Damgaard, Schmock, Henriette, Skjødt, Celina, Rosengren, Anders, Høffding, Louise.K.Enggaard, Thygesen, Johan Hilge, Werge, Thomas Mears, Derks, Eske M, Vorstman, Jacob A S, Ripke, Stephan, Kahn, Rene S, Ophoff, Roel A, Hansen, Thomas, Olsen, Line, Jakobsen, Klaus Damgaard, Schmock, Henriette, Skjødt, Celina, Rosengren, Anders, Høffding, Louise.K.Enggaard, Thygesen, Johan Hilge, and Werge, Thomas Mears

Abstract

The presence of subclinical levels of psychosis in the general population may imply that schizophrenia is the extreme expression of more or less continuously distributed traits in the population. In a previous study, we identified five quantitative measures of schizophrenia (positive, negative, disorganisation, mania, and depression scores). The aim of this study is to examine the association between a direct measure of genetic risk of schizophrenia and the five quantitative measures of psychosis. Estimates of the log of the odds ratios of case/control allelic association tests were obtained from the Psychiatric GWAS Consortium (PGC) (minus our sample) which included genome-wide genotype data of 8,690 schizophrenia cases and 11,831 controls. These data were used to calculate genetic risk scores in 314 schizophrenia cases and 148 controls from the Netherlands for whom genotype data and quantitative symptom scores were available. The genetic risk score of schizophrenia was significantly associated with case-control status (p

Published
2012

22. Genome-wide association study of clinical dimensions of schizophrenia:polygenic effect on disorganized symptoms

Author

Fanous, Ayman H, Zhou, Baiyu, Aggen, Steven H, Bergen, Sarah E, Amdur, Richard L, Duan, Jubao, Sanders, Alan R, Shi, Jianxin, Mowry, Bryan J, Olincy, Ann, Amin, Farooq, Cloninger, C Robert, Silverman, Jeremy M, Buccola, Nancy G, Byerley, William F, Black, Donald W, Freedman, Robert, Dudbridge, Frank, Holmans, Peter A, Ripke, Stephan, Gejman, Pablo V, Kendler, Kenneth S, Levinson, Douglas F, Hansen, Thomas Folkmann, Werge, Thomas Mears, Olsen, Line, Rasmussen, Henrik Berg, Fanous, Ayman H, Zhou, Baiyu, Aggen, Steven H, Bergen, Sarah E, Amdur, Richard L, Duan, Jubao, Sanders, Alan R, Shi, Jianxin, Mowry, Bryan J, Olincy, Ann, Amin, Farooq, Cloninger, C Robert, Silverman, Jeremy M, Buccola, Nancy G, Byerley, William F, Black, Donald W, Freedman, Robert, Dudbridge, Frank, Holmans, Peter A, Ripke, Stephan, Gejman, Pablo V, Kendler, Kenneth S, Levinson, Douglas F, Hansen, Thomas Folkmann, Werge, Thomas Mears, Olsen, Line, and Rasmussen, Henrik Berg

Abstract

Multiple sources of evidence suggest that genetic factors influence variation in clinical features of schizophrenia. The authors present the first genome-wide association study (GWAS) of dimensional symptom scores among individuals with schizophrenia.

Published
2012

23. Don't give up on GWAS

Author

Sullivan, P, Werge, Thomas Mears, Sullivan, P, and Werge, Thomas Mears

Published
2012

24. Runs of homozygosity implicate autozygosity as a schizophrenia risk factor

Author

Keller, Matthew C, Simonson, Matthew A, Ripke, Stephan, Neale, Ben M, Gejman, Pablo V, Howrigan, Daniel P, Lee, Sang Hong, Lencz, Todd, Levinson, Douglas F, Sullivan, Patrick F, Hansen, Thomas, Ingason, Andrés, Olsen, Line, Schmock, Henriette, Skjødt, Celina, Thygesen, Johan Hilge, Rosengren, Anders, Werge, Thomas Mears, Keller, Matthew C, Simonson, Matthew A, Ripke, Stephan, Neale, Ben M, Gejman, Pablo V, Howrigan, Daniel P, Lee, Sang Hong, Lencz, Todd, Levinson, Douglas F, Sullivan, Patrick F, Hansen, Thomas, Ingason, Andrés, Olsen, Line, Schmock, Henriette, Skjødt, Celina, Thygesen, Johan Hilge, Rosengren, Anders, and Werge, Thomas Mears

Abstract

Autozygosity occurs when two chromosomal segments that are identical from a common ancestor are inherited from each parent. This occurs at high rates in the offspring of mates who are closely related (inbreeding), but also occurs at lower levels among the offspring of distantly related mates. Here, we use runs of homozygosity in genome-wide SNP data to estimate the proportion of the autosome that exists in autozygous tracts in 9,388 cases with schizophrenia and 12,456 controls. We estimate that the odds of schizophrenia increase by ~17% for every 1% increase in genome-wide autozygosity. This association is not due to one or a few regions, but results from many autozygous segments spread throughout the genome, and is consistent with a role for multiple recessive or partially recessive alleles in the etiology of schizophrenia. Such a bias towards recessivity suggests that alleles that increase the risk of schizophrenia have been selected against over evolutionary time.

Published
2012

25. Utility and adoption of CYP2D6 and CYP2C19 genotyping and its translation into psychiatric clinical practice

Author

Jürgens, G, Jacobsen, C B, Rasmussen, H B, Werge, T, Nordentoft, M, Andersen, S E, Werge, Thomas Mears, Jürgens, G, Jacobsen, C B, Rasmussen, H B, Werge, T, Nordentoft, M, Andersen, S E, and Werge, Thomas Mears

Abstract

To describe clinical utility and adoption of routinely offered CYP2D6 and CYP2C19 genotyping (CYP test) in daily clinical practice of a psychiatric centre.

Published
2012

26. Lack of association between two dopamine D2 receptor gene polymorphisms and schizophrenia

Author

Caprini, Sara, Saetre, Peter, Melle, Ingrid, Djurovic, Srdjan, Andreassen, Ole A, Skjødt, Celina, Doung, Linh, Werge, Thomas Mears, Hall, Hakan, Agartz, Ingrid, Terenius, Lars, Jönsson, Erik G, Caprini, Sara, Saetre, Peter, Melle, Ingrid, Djurovic, Srdjan, Andreassen, Ole A, Skjødt, Celina, Doung, Linh, Werge, Thomas Mears, Hall, Hakan, Agartz, Ingrid, Terenius, Lars, and Jönsson, Erik G

Published
2011

27. Genome-wide association study identifies four loci associated with eruption of permanent teeth

Author

Geller, Frank, Feenstra, Bjarke, Zhang, Hao, Shaffer, John R, Hansen, Thomas, Esserlind, Ann-Louise, Boyd, Heather A, Nohr, Ellen A, Timpson, Nicholas J, Fatemifar, Ghazaleh, Paternoster, Lavinia, Evans, David M, Weyant, Robert J, Levy, Steven M, Lathrop, Mark, Smith, George Davey, Murray, Jeffrey C, Olesen, Jes, Werge, Thomas Mears, Marazita, Mary L, Sørensen, Thorkild I A, Melbye, Mads, Geller, Frank, Feenstra, Bjarke, Zhang, Hao, Shaffer, John R, Hansen, Thomas, Esserlind, Ann-Louise, Boyd, Heather A, Nohr, Ellen A, Timpson, Nicholas J, Fatemifar, Ghazaleh, Paternoster, Lavinia, Evans, David M, Weyant, Robert J, Levy, Steven M, Lathrop, Mark, Smith, George Davey, Murray, Jeffrey C, Olesen, Jes, Werge, Thomas Mears, Marazita, Mary L, Sørensen, Thorkild I A, and Melbye, Mads

Abstract

The sequence and timing of permanent tooth eruption is thought to be highly heritable and can have important implications for the risk of malocclusion, crowding, and periodontal disease. We conducted a genome-wide association study of number of permanent teeth erupted between age 6 and 14 years, analyzed as age-adjusted standard deviation score averaged over multiple time points, based on childhood records for 5,104 women from the Danish National Birth Cohort. Four loci showed association at P

Published
2011

29. Suicidal Behavior and the Serotonin Transporter Gene Polymorphism (5-HTTLPR) with Novel Subtypes, in Danish Schizophrenic Patients

Author

Wang, August Gabriel, Rasmussen, Henrik Berg, Sørensen, Holger Jelling, Hvid, Marianne, Breddam, Claus Henrik, Hansen, Bjarne, Bille, Vibeke Høg, Garsdal, Ole, Jacoby, Anne, Søbye, Karen, Dam, Ole Henrik, Krogsbøl, Henrik, Timm, Sally, Werge, Thomas Mears, Wang, August Gabriel, Rasmussen, Henrik Berg, Sørensen, Holger Jelling, Hvid, Marianne, Breddam, Claus Henrik, Hansen, Bjarne, Bille, Vibeke Høg, Garsdal, Ole, Jacoby, Anne, Søbye, Karen, Dam, Ole Henrik, Krogsbøl, Henrik, Timm, Sally, and Werge, Thomas Mears

Published
2009

30. The prevalence and early life determinants of mental disorders in school aged children: 11 years follow up of the CCC 2000 birth cohort study. Poster presentation XVII.ESCAP International Congress Budapest August 2009

Author

Jeppesen, Pia, Fagerlund, Birgitte, Glenthøj, Birte Yding, Werge, Thomas Mears, Linneberg, Allan, Jørgensen, Torben, Skovgaard, Anne Mette, Jeppesen, Pia, Fagerlund, Birgitte, Glenthøj, Birte Yding, Werge, Thomas Mears, Linneberg, Allan, Jørgensen, Torben, and Skovgaard, Anne Mette

Published
2009

31. The impact of CYP2D6 and CYP2C19 polymorphisms on suicidal behavior and substance abuse disorder among patients with schizophrenia: a retrospective study

Author

Kobylecki, C.J., Hansen, T., Timm, S., Wang, August Gabriel, Jakobsen, K.D., Sørensen, Holger Jelling, Rasmussen, Henrik Barner, Werge, Thomas Mears, Kobylecki, Camilla J, Hansen, Thomas Folkmann, Timm, Sally, Wang, August, Jakobsen, Klaus D, Sørensen, Holger J, Rasmussen, Henrik B, Werge, Thomas, Kobylecki, C.J., Hansen, T., Timm, S., Wang, August Gabriel, Jakobsen, K.D., Sørensen, Holger Jelling, Rasmussen, Henrik Barner, Werge, Thomas Mears, Kobylecki, Camilla J, Hansen, Thomas Folkmann, Timm, Sally, Wang, August, Jakobsen, Klaus D, Sørensen, Holger J, Rasmussen, Henrik B, and Werge, Thomas

Abstract

Suicidal behavior and substance abuse are frequent phenomena among patients with schizophrenia and may be attributable in part to antipsychotic treatment failure. Individuals who carry functional variants of the CYP2D6 and CYP2C9 genes, shown to cause altered drug metabolism of psychoactive drugs, are at risk of toxic accumulation or rapid elimination of these drugs, leading to treatment failure. We tested whether substance abuse disorder and suicidal behavior were associated with the CYP2D6 and CYP2C9 genotypes among patients with schizophrenia. Three hundred sixty-two patients with schizophrenia spectrum disorders (International Classification of Diseases, 10th Revision) were genotyped for functional CYP2D6 and CYP2C19 polymorphisms. Based on available medical records and clinical interviews, their suicidal behavior and substance abuse disorder were evaluated. No significant associations between the CYP2D6 and CYP2C19 genotypes and suicidal behavior or substance abuse disorder were noted, and we conclude that cytochrome P450 genotyping in its present form is clinically irrelevant with respect to these phenomena Udgivelsesdato: 2008, Suicidal behavior and substance abuse are frequent phenomena among patients with schizophrenia and may be attributable in part to antipsychotic treatment failure. Individuals who carry functional variants of the CYP2D6 and CYP2C19 genes, shown to cause altered drug metabolism of psychoactive drugs, are at risk of toxic accumulation or rapid elimination of these drugs, leading to treatment failure. We tested whether substance abuse disorder and suicidal behavior were associated with the CYP2D6 and CYP2C19 genotypes among patients with schizophrenia. Three hundred sixty-two patients with schizophrenia spectrum disorders (International Classification of Diseases, 10th Revision) were genotyped for functional CYP2D6 and CYP2C19 polymorphisms. Based on available medical records and clinical interviews, their suicidal behavior and substance abuse disorder were evaluated. No significant associations between the CYP2D6 and CYP2C19 genotypes and suicidal behavior or substance abuse disorder were noted, and we conclude that cytochrome P450 genotyping in its present form is clinically irrelevant with respect to these phenomena.

Published
2008

35. The estrogen hypothesis of schizophrenia implicates glucose metabolism: association study in three independent samples

Author

Olsen, Line, Hansen, Thomas, Jakobsen, Klaus D., Djurovic, Srdjan, Melle, Ingrid, Agartz, Ingrid, Hall, Haakon, Ullum, H., Timm, S., Wang, August Gabriel, Jonsson, Erik G., Andreassen, Ole A., Werge, Thomas Mears, Olsen, Line, Hansen, Thomas, Jakobsen, Klaus D., Djurovic, Srdjan, Melle, Ingrid, Agartz, Ingrid, Hall, Haakon, Ullum, H., Timm, S., Wang, August Gabriel, Jonsson, Erik G., Andreassen, Ole A., and Werge, Thomas Mears

Abstract

BACKGROUND: Schizophrenia is a highly heritable complex psychiatric disorder with an underlying pathophysiology that is still not well understood. Metaanalyses of schizophrenia linkage studies indicate numerous but rather large disease-associated genomic regions, whereas accumulating gene- and protein expression studies have indicated an equally large set of candidate genes that only partially overlap linkage genes. A thorough assessment, beyond the resolution of current GWA studies, of the disease risk conferred by the numerous schizophrenia candidate genes is a daunting and presently not feasible task. We undertook these challenges by using an established clinical paradigm, the estrogen hypothesis of schizophrenia, as the criterion to select candidates among the numerous genes experimentally implicated in schizophrenia. Bioinformatic tools were used to build and priorities the signaling networks implicated by the candidate genes resulting from the estrogen selection. We identified ten candidate genes using this approach that are all active in glucose metabolism and particularly in the glycolysis. Thus, we tested the hypothesis that variants of the glycolytic genes are associated with schizophrenia or at least with gender-associated aspects of the illness. RESULTS: We genotyped 185 SNPs in three independent case-control samples of Scandinavian origin (a total of 765 patients and 1274 control subjects). Variants of the mitogen-activated protein kinase 14 gene (MAPK14) and the phosphoenolpyruvate carboxykinase 1 (PCK1) and fructose-1,6-biphosphatase (FBP1) were nominal significantly associated with schizophrenia, and several haplotypes within enolase 2 gene (ENO2) consist of the same SNP allele having elevated risk of schizophrenia. Importantly, we find no evidence of stratification due to nationality or gender. CONCLUSION: Several gene variants in the Glycolysis were associated with schizophrenia in three independent samples. However, the findings are weak and not r

Published
2008

36. Analysis of heterogeneity and epistasis in physiological mixed populations by combined structural equation modelling and latent class analysis

Author

Fenger, Mogens, Linneberg, A., Werge, Thomas Mears, Jørgensen, Torben, Fenger, Mogens, Linneberg, A., Werge, Thomas Mears, and Jørgensen, Torben

Abstract

Udgivelsesdato: 2008-null, BACKGROUND: Biological systems are interacting, molecular networks in which genetic variation contributes to phenotypic heterogeneity. This heterogeneity is traditionally modelled as a dichotomous trait (e.g. affected vs. non-affected). This is far too simplistic considering the complexity and genetic variations of such networks. METHODS: In this study on type 2 diabetes mellitus, heterogeneity was resolved in a latent class framework combined with structural equation modelling using phenotypic indicators of distinct physiological processes. We modelled the clinical condition "the metabolic syndrome", which is known to be a heterogeneous and polygenic condition with a clinical endpoint (type 2 diabetes mellitus). In the model presented here, genetic factors were not included and no genetic model is assumed except that genes operate in networks. The impact of stratification of the study population on genetic interaction was demonstrated by analysis of several genes previously associated with the metabolic syndrome and type 2 diabetes mellitus. RESULTS: The analysis revealed the existence of 19 distinct subpopulations with a different propensity to develop diabetes mellitus within a large healthy study population. The allocation of subjects into subpopulations was highly accurate with an entropy measure of nearly 0.9. Although very few gene variants were directly associated with metabolic syndrome in the total study sample, almost one third of all possible epistatic interactions were highly significant. In particular, the number of interactions increased after stratifying the study population, suggesting that interactions are masked in heterogenous populations. In addition, the genetic variance increased by an average of 35-fold when analysed in the subpopulations. CONCLUSION: The major conclusions from this study are that the likelihood of detecting true association between genetic variants and complex traits increases tremendously when studied in physiological homog

Published
2008

37. Reliability of clinical ICD-10 diagnoses among electroconvulsive therapy patients with chronic affective disorders

Author

Jakobsen, Klaus Damgaard, Hansen, Thomas Folkmann, Dam, Henrik, Larsen, Ejner Bundgaard, Gether, Ulrik, Werge, Thomas Mears, Jakobsen, Klaus Damgaard, Hansen, Thomas Folkmann, Dam, Henrik, Larsen, Ejner Bundgaard, Gether, Ulrik, and Werge, Thomas Mears

Abstract

Background and Objectives: Diagnostic reliability is of major concern both to clinicians and researchers. The aim has been to investigate the trustworthiness of clinical ICD-10 affective disorder diagnoses for research purpose. Methods: 150 ECT patients with chronic affective disorders were investigated. A standardized schema for basic anamnesis and the Operational Criteria Checklist for Psychotic and Affective Illness (OPCRIT) were used. The sensitivity, specificity, positive and negative predictive values of clinical affective disorder ICD-10 diagnoses and the formal agreement between clinical ICD-10, OPCRIT ICD-10 and DSM-IV diagnoses were determined using unweighted K-statistics. Results: The sensitivity, specificity, positive and negative predictive values of the clinical bipolar diagnoses was 0.55, 0.75, 0.42 and 0.84, respectively. The sensitivity, specificity, positive and negative predictive values of the clinical unipolar diagnoses was 0.79, 0.55, 0.77 and 0.58, respectively. The agreement between clinical ICD-10 and OPCRIT ICD-10 bipolar vs. non-bipolar diagnoses was low, K = 0.28. The agreement between clinical ICD-10 and OPCRIT ICD-10 unipolar vs. non-unipolar diagnoses was low, K = 0.35. The agreement between OPCRIT ICD-10 and DSM-IV diagnoses, on bipolar vs. non-bipolar disorders was high, K = 0.91, and the agreement on unipolar vs. non-unipolar disorders was fairly high, K = 0.78. Conclusions: This study demonstrates that the reliability of clinical ICD-10 diagnoses of affective disorders from chronic subjects with a history of ECT is problematic despite sample homogeneity on basic clinical, demographic and epidemiological parameters Udgivelsesdato: 2008

Published
2008

38. GABA(A) receptor function is regulated by lipid bilayer elasticity

Author

Søgaard, Rikke, Werge, Thomas Mears, Bertelsen, Camilla, Lundbye, Camilla, Madsen, Kenneth L, Nielsen, Claus H, Lundbaek, Jens A, Søgaard, Rikke, Werge, Thomas Mears, Bertelsen, Camilla, Lundbye, Camilla, Madsen, Kenneth L, Nielsen, Claus H, and Lundbaek, Jens A

Abstract

Udgivelsesdato: 2006-Oct-31, Docosahexaenoic acid (DHA) and other polyunsaturated fatty acids (PUFAs) promote GABA(A) receptor [(3)H]-muscimol binding, and DHA increases the rate of GABA(A) receptor desensitization. Triton X-100, a structurally unrelated amphiphile, similarly promotes [(3)H]-muscimol binding. The mechanism(s) underlying these effects are poorly understood. DHA and Triton X-100, at concentrations that affect GABA(A) receptor function, increase the elasticity of lipid bilayers measured as decreased bilayer stiffness using gramicidin channels as molecular force transducers. We have previously shown that membrane protein function can be regulated by amphiphile-induced changes in bilayer elasticity and hypothesized that GABA(A) receptors could be similarly regulated. We therefore studied the effects of four structurally unrelated amphiphiles that decrease bilayer stiffness (Triton X-100, octyl-beta-glucoside, capsaicin, and DHA) on GABA(A) receptor function in mammalian cells. All the compounds promoted GABA(A) receptor [(3)H]-muscimol binding by increasing the binding capacity of high-affinity binding without affecting the associated equilibrium binding constant. A semiquantitative analysis found a similar quantitative relation between the effects on bilayer stiffness and [(3)H]-muscimol binding. Membrane cholesterol depletion, which also decreases bilayer stiffness, similarly promoted [(3)H]-muscimol binding. In whole-cell voltage-clamp experiments, Triton X-100, octyl-beta-glucoside, capsaicin, and DHA all reduced the peak amplitude of the GABA-induced currents and increased the rate of receptor desensitization. The effects of the amphiphiles did not correlate with the expected changes in monolayer spontaneous curvature. We conclude that GABA(A) receptor function is regulated by lipid bilayer elasticity. PUFAs may generally regulate membrane protein function by affecting the elasticity of the host lipid bilayer.

Published
2006

39. Identifikation af markører for vigtige behandlingsudfald i elektroniske patientjournaler for patienter på Psykiatrisk Center Sct. Hans med psykiatriske diagnoser hvor behandling med antipsykotika er indiceret

Author

Klitgaard, Kasper, Bulskov, Henrik, Werge, Thomas Mears, and Vang, Ole

Subjects
k-medoids, EPJ, skizofreni, behandlingsudfald, Sct. Hans, antipsykotika, elektronisk patientjournal, data mining, monoterapi, clustering
Abstract

I løbet af indlæggelsen på Psykiatrisk Center Sct. Hans indsamles informationer fra behandlingsforløbet i den elektroniske patientjournal (EPJ). Ud fra en hypotese om, at udvalgte parametre blandt de journalførte informationer udgør markører for det pågældende behandlingsudfald, forsøges disse markører fastlagt i et retrospektivt kohorte-studie af 354 psykiatriske patienter med behandlingsudfaldene udskrivning (n = 224) og behandlingsskifte (n = 130) på baggrund af behandlingsforløb i antipsykotisk monoterapi i minimum 4 uger. Fastlæggelsen af markører sker i tilfælde af stærk overensstemmelse (k > 0,6) imellem to uafhængige fordelinger af samme kohorte; (1) opdelingen af patientkohorten i to grupper på baggrund af behandlingsudfaldet (forventet fordeling); (2) opdelingen af patientkohorten ved k-medoids clustering af udvalgte parametre (observeret fordeling). Trods gentagne undersøgelser med clusterfordelinger baseret på forskellige kliniske variable og selektionssnit af journalnotater opnåedes kun svag overensstemmelse (k

Published
2009

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