Your search keyword '"Zoltán Bochdanovits"' showing total 36 results

1. Correction: Modulatory Effects of the Piccolo Genotype on Emotional Memory in Health and Depression.

Author

Saskia Woudstra, Marie-José van Tol, Zoltán Bochdanovits, Nic J. van der Wee, Frans G. Zitman, Mark A. van Buchem, Esther M. Opmeer, André Aleman, Brenda W. Penninx, Dick J. Veltman, and Witte J. Hoogendijk

Subjects

Medicine, Science

Published

2013

2. Resequencing three candidate genes for major depressive disorder in a Dutch cohort.

Author

Eva C Verbeek, Marianna R Bevova, Zoltán Bochdanovits, Patrizia Rizzu, Ingrid M C Bakker, Tiny Uithuisje, Eco J De Geus, Johannes H Smit, Brenda W Penninx, Dorret I Boomsma, Witte J G Hoogendijk, and Peter Heutink

Subjects

Medicine, Science

Abstract

Major depressive disorder (MDD) is a psychiatric disorder, characterized by periods of low mood of more than two weeks, loss of interest in normally enjoyable activities and behavioral changes. MDD is a complex disorder and does not have a single genetic cause. In 2009 a genome wide association study (GWAS) was performed on the Dutch GAIN-MDD cohort. Many of the top signals of this GWAS mapped to a region spanning the gene PCLO, and the non-synonymous coding single nucleotide polymorphism (SNP) rs2522833 in the PCLO gene became genome wide significant after post-hoc analysis. We performed resequencing of PCLO, GRM7, and SLC6A4 in 50 control samples from the GAIN-MDD cohort, to detect new genomic variants. Subsequently, we genotyped these variants in the entire GAIN-MDD cohort and performed association analysis to investigate if rs2522833 is the causal variant or simply in linkage disequilibrium with a more associated variant. GRM7 and SLC6A4 are both candidate genes for MDD from literature. We aimed to gather more evidence that rs2522833 is indeed the causal variant in the GAIN-MDD cohort or to find a previously undetected common variant in either PCLO, GRM7, or SLC6A4 with a higher association in this cohort. After next generation sequencing and association analysis we excluded the possibility of an undetected common variant to be more associated. For neither PCLO nor GRM7 we found a more associated variant. For SLC6A4, we found a new SNP that showed a lower P-value (P = 0.07) than in the GAIN-MDD GWAS (P = 0.09). However, no evidence for genome-wide significance was found. Although we did not take into account rare variants, we conclude that our results provide further support for the hypothesis that the non-synonymous coding SNP rs2522833 in the PCLO gene is indeed likely to be the causal variant in the GAIN-MDD cohort.

Published

2013

3. Modulatory effects of the piccolo genotype on emotional memory in health and depression.

Author

Saskia Woudstra, Marie-José van Tol, Zoltán Bochdanovits, Nic J van der Wee, Frans G Zitman, Mark A van Buchem, Esther M Opmeer, André Aleman, Brenda W Penninx, Dick J Veltman, and Witte J Hoogendijk

Subjects

Medicine, Science

Abstract

Major depressive disorder (MDD) has been associated with biased memory formation for mood-congruent information, which may be related to altered monoamine levels. The piccolo (PCLO) gene, involved in monoaminergic neurotransmission, has previously been linked to depression in a genome-wide association study. Here, we investigated the role of the PCLO risk allele on functional magnetic resonance imaging (MRI) correlates of emotional memory in a sample of 89 MDD patients (64 PCLO risk allele carriers) and 29 healthy controls (18 PCLO risk allele carriers). During negative word encoding, risk allele carriers showed significant lower activity relative to non-risk allele carriers in the insula, and trend-wise in the anterior cingulate cortex and inferior frontal gyrus. Moreover, depressed risk allele carriers showed significant lower activity relative to non-risk allele carriers in the striatum, an effect which was absent in healthy controls. Finally, amygdalar response during processing new positive words vs. known words was blunted in healthy PCLO+ carriers and in MDD patients irrespective of genotype, which may indicate that signalling of salient novel information does not occur to the same extent in PCLO+ carriers and MDD patients. The PCLO risk allele may increase vulnerability for MDD by modulating local brain function with regard to responsiveness to salient stimuli (i.e. insula) and processing novel negative information. Also, depression-specific effects of PCLO on dorsal striatal activation during negative word encoding and the absence of amygdalar salience signalling for novel positive information further suggest a role of PCLO in symptom maintenance in MDD.

Published

2013

4. A fine-mapping study of 7 top scoring genes from a GWAS for major depressive disorder.

Author

Eva C Verbeek, Ingrid M C Bakker, Marianna R Bevova, Zoltán Bochdanovits, Patrizia Rizzu, David Sondervan, Gonneke Willemsen, Eco J de Geus, Johannes H Smit, Brenda W Penninx, Dorret I Boomsma, Witte J G Hoogendijk, and Peter Heutink

Subjects

Medicine, Science

Abstract

Major depressive disorder (MDD) is a psychiatric disorder that is characterized--amongst others--by persistent depressed mood, loss of interest and pleasure and psychomotor retardation. Environmental circumstances have proven to influence the aetiology of the disease, but MDD also has an estimated 40% heritability, probably with a polygenic background. In 2009, a genome wide association study (GWAS) was performed on the Dutch GAIN-MDD cohort. A non-synonymous coding single nucleotide polymorphism (SNP) rs2522833 in the PCLO gene became only nominally significant after post-hoc analysis with an Australian cohort which used similar ascertainment. The absence of genome-wide significance may be caused by low SNP coverage of genes. To increase SNP coverage to 100% for common variants (m.a.f.>0.1, r(2)>0.8), we selected seven genes from the GAIN-MDD GWAS: PCLO, GZMK, ANPEP, AFAP1L1, ST3GAL6, FGF14 and PTK2B. We genotyped 349 SNPs and obtained the lowest P-value for rs2715147 in PCLO at P = 6.8E-7. We imputed, filling in missing genotypes, after which rs2715147 and rs2715148 showed the lowest P-value at P = 1.2E-6. When we created a haplotype of these SNPs together with the non-synonymous coding SNP rs2522833, the P-value decreased to P = 9.9E-7 but was not genome wide significant. Although our study did not identify a more strongly associated variant, the results for PCLO suggest that the causal variant is in high LD with rs2715147, rs2715148 and rs2522833.

Published

2012

5. Comprehensive mRNA expression profiling distinguishes tauopathies and identifies shared molecular pathways.

Author

Iraad F Bronner, Zoltán Bochdanovits, Patrizia Rizzu, Wouter Kamphorst, Rivka Ravid, John C van Swieten, and Peter Heutink

Subjects

Medicine, Science

Abstract

BACKGROUND:Understanding the aetiologies of neurodegenerative diseases such as Alzheimer's disease (AD), Pick's disease (PiD), Progressive Supranuclear Palsy (PSP) and Frontotemporal dementia (FTD) is often hampered by the considerable clinical and molecular overlap between these diseases and normal ageing. The development of high throughput genomic technologies such as microarrays provide a new molecular tool to gain insight in the complexity and relationships between diseases, as they provide data on the simultaneous activity of multiple genes, gene networks and cellular pathways. METHODOLOGY/PRINCIPAL FINDINGS:We have constructed genome wide expression profiles from snap frozen post-mortem tissue from the medial temporal lobe of patients with four neurodegenerative disorders (5 AD, 5 PSP, 5 PiD and 5 FTD patients) and 5 control subjects. All patients were matched for age, gender, ApoE-epsilon and MAPT (tau) haplotype. From all groups a total of 790 probes were shown to be differently expressed when compared to control individuals. The results from these experiments were then used to investigate the correlations between clinical, pathological and molecular findings. From the 790 identified probes we extracted a gene set of 166 probes whose expression could discriminate between these disorders and normal ageing. CONCLUSIONS/SIGNIFICANCE:From genome wide expression profiles we extracted a gene set of 166 probes whose expression could discriminate between neurological disorders and normal ageing. This gene set can be further developed into an accurate microarray-based classification test. Furthermore, from this dataset we extracted a disease specific set of genes and identified two aging related transcription factors (FOXO1A and FOXO3A) as possible drug targets related to neurodegenerative disease.

Published

2009

6. Variation at GRN 3'-UTR rs5848 is not associated with a risk of frontotemporal lobar degeneration in Dutch population.

Author

Javier Simón-Sánchez, Harro Seelaar, Zoltán Bochdanovits, Dorly J H Deeg, John C van Swieten, and Peter Heutink

Subjects

Medicine, Science

Abstract

A single nucleotide polymorphism (rs5848) located in the 3'- untranslated region of GRN has recently been associated with a risk of frontotemporal lobar degeneration (FTLD) in North American population particularly in pathologically confirmed cases with neural inclusions immunoreactive for ubiquitin and TAR DNA-binding protein 43 (TDP-43), but negative for tau and alpha-synuclein (FTLD-TDP).In an effort to replicate these results in a different population, rs5848 was genotyped in 256 FTLD cases and 1695 controls from the Netherlands. Single SNP gender-adjusted logistic regression analysis revealed no significant association between variation at rs5848 and FTLD. Fisher's exact test, failed to find any significant association between rs5848 and a subset of 23 pathology confirmed FTLD-TDP cases.The evidence presented here suggests that variation at rs5848 does not contribute to the etiology of FTLD in the Dutch population.

Published

2009

7. Genome-wide prediction of functional gene-gene interactions inferred from patterns of genetic differentiation in mice and men.

Author

Zoltán Bochdanovits, David Sondervan, Sophie Perillous, Toos van Beijsterveldt, Dorret Boomsma, and Peter Heutink

Subjects

Medicine, Science

Abstract

The human genome encodes a limited number of genes yet contributes to individual differences in a vast array of heritable traits. A possible explanation for the capacity our genome to generate this virtually unlimited range of phenotypic variation in complex traits is to assume functional interactions between genes. Therefore we searched two mammalian genomes to identify potential epistatic interactions by looking for co-adapted genes marked by excess two-locus genetic differentiation between populations/lineages using publicly available SNP genotype data. The practical motivation for this effort is to reduce the number of pair-wise tests that need to be performed in genome-wide association studies aimed at detecting GxG interactions, by focusing on pairs predicted to be more likely to jointly affect variation in complex traits. Hence, this approach generates a list of candidate interactions that can be empirically tested. In both the mouse and human data we observed two-locus genetic differentiation in excess of what can be expected from chance alone based on simulations. In an attempt to validate our hypothesis that pairs of genes showing excess genetic divergence represent potential functional interactions, we selected a small set of gene combinations postulated to be interacting based on our analyses and looked for a combined effect of the selected genes on variation in complex traits in both mice and man. In both cases the individual effect of the genes were not significant, instead we observed marginally significant interaction effects. These results show that genome wide searches for gene-gene interactions based on population genetic data are feasible and can generate interesting candidate gene pairs to be further tested for their contribution to phenotypic variation in complex traits.

Published

2008

8. Unbiased screen for interactors of leucine-rich repeat kinase 2 supports a common pathway for sporadic and familial Parkinson disease

Author

Mina Ryten, Daniah Trabzuni, J. Ding, Bart Post, Albert Hofman, Jean-Charles Lambert, Olaf Riess, Michele T.M. Hu, Andrew B. Singleton, Stephen Sawcer, X. Huang, Caroline H. Williams-Gray, H. R. Zielke, C Smith, Peter Lichtner, B.P.C. van de Warrenburg, Bernard Ravina, F. Durif, Ellen Sidransky, Mike A. Nalls, Karen E. Morrison, J. R. Gibbs, Robert L. Johnson, Peter Heutink, David J. Burn, Michael Bonin, Sarah Edkins, T. Gasser, Luigi Ferrucci, H. Chau, Sampath Arepalli, Chris C. A. Spencer, Yoav Ben-Shlomo, Honglei Chen, Caroline M. Tanner, Zoltán Bochdanovits, Ruth Chia, Heiko Huber, Kari Stefansson, Dena G. Hernandez, Jean-Marc Taymans, Veerle Baekelandt, Iakov N. Rudenko, Evy Lobbestael, Huw R. Morris, A. Goate, C. Moorby, Lois E. Greene, Manu Sharma, Emma Gray, Ira Shoulson, Janet Brooks, Juan C. Troncoso, K. Shaw, Laura Civiero, Alessandra Biffi, Hans Scheffer, Matthew Moore, Alan B. Zonderman, S. Sveinbjornsdottir, Avazeh Tashakkori-Ghanbaria, Jean-Christophe Corvol, Vincent Plagnol, H. Petursson, Alice Kaganovich, M M Wickremaratchi, Nigel Williams, Thomas Foltynie, Henk W. Berendse, P. Damier, A. Strange, J. M. Cooper, Simon C. Potter, Patricia Limousin, Jiali Gao, Sophie Winder-Rhodes, M. Van Der Brug, Marie Vidailhet, Elisa Greggio, Nicholas W. Wood, Kevin Talbot, M. R. Cookson, Johanna Huttenlocher, J.J. van Hilten, Dan L. Longo, Alisdair McNeill, François Tison, K.D. van Dijk, David N. Hauser, Allissa Dillman, Suneil K. Kalia, Lorraine V. Kalia, Patrick F. Chinnery, Alexis Brice, Kelechi Ndukwe, J. F. Dartigues, M. Gardner, Mohamad Saad, Palmi V. Jonsson, Kailash P. Bhatia, Roger A. Barker, André G. Uitterlinden, Maria Martinez, R. Walker, Elisa Majounie, Fernando Rivadeneira, Joel S. Perlmutter, Panagiotis Deloukas, Bryan J. Traynor, Ese E. Mudanohwo, Grisel Lopez, UM Sheerin, Joanne D. Stockton, Thomas Illig, Andres M. Lozano, Rita Guerreiro, David T. Dexter, Andrew J. Lees, Sean Chong, Gavin Hudson, Cordelia Langford, Günther Deuschl, Ravindran Kumaran, Janice L. Holton, Tamas Revesz, B.R. Bloem, Alexandra Beilina, Clare Elizabeth Harris, Daniela Berg, Anthony H.V. Schapira, Suzanne Lesage, Sean S. O'Sullivan, Albert R. Hollenbeck, James A. Pearson, R. M. A. de Bie, Delia Lorenz, Sarah E. Hunt, Richard O'Brien, Gavin Charlesworth, Maciej B. Olszewski, Stacy Steinberg, Kathrin Brockmann, Carl E Clarke, Patrizia Rizzu, Claudia Schulte, Hreinn Stefansson, Daan C. Velseboer, Omar Gustafsson, Jonathan R. Evans, Alexandra Durr, Javier Simón-Sánchez, Pierre Pollak, H. Z. Munchen, Jose Bras, Carl Counsell, John Hardy, ANS - Amsterdam Neuroscience, Neurology, and Graduate School

Subjects

Candidate gene, autophagy, Blotting, Western, Golgi Apparatus, Genome-wide association study, Protein Serine-Threonine Kinases, Biology, Leucine-rich repeat, Cell Fractionation, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Mass Spectrometry, Commentaries, Protein Interaction Mapping, Humans, Immunoprecipitation, Genetic Predisposition to Disease, Transport Vesicles, Gene, Adaptor Proteins, Signal Transducing, DNA Primers, Genetics, Analysis of Variance, Microscopy, Confocal, Multidisciplinary, Kinase, HEK 293 cells, BAG5, Intracellular Signaling Peptides and Proteins, Brain, rab7 GTP-Binding Proteins, Signal transducing adaptor protein, Parkinson Disease, Biological Sciences, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], GAK, LRRK2, nervous system diseases, HEK293 Cells, Genetic Loci, rab GTP-Binding Proteins, Multiprotein Complexes, trans-Golgi, Genome-Wide Association Study, Plasmids

Abstract

Item does not contain fulltext Mutations in leucine-rich repeat kinase 2 (LRRK2) cause inherited Parkinson disease (PD), and common variants around LRRK2 are a risk factor for sporadic PD. Using protein-protein interaction arrays, we identified BCL2-associated athanogene 5, Rab7L1 (RAB7, member RAS oncogene family-like 1), and Cyclin-G-associated kinase as binding partners of LRRK2. The latter two genes are candidate genes for risk for sporadic PD identified by genome-wide association studies. These proteins form a complex that promotes clearance of Golgi-derived vesicles through the autophagy-lysosome system both in vitro and in vivo. We propose that three different genes for PD have a common biological function. More generally, data integration from multiple unbiased screens can provide insight into human disease mechanisms.

Published

2014

9. Accurate prediction of a minimal region around a genetic association signal that contains the causal variant

Author

Zoltán Bochdanovits, Peter Heutink, Aad van der Vaart, Witte J.G. Hoogendijk, Javier Simón-Sánchez, Marianne A. Jonker, Psychiatry, Functional Genomics, Mathematics, Neuroscience Campus Amsterdam - Neurodegeneration, Human genetics, and NCA - neurodegeneration

Subjects

Genetics, Linkage disequilibrium, Candidate gene, Models, Genetic, Association (object-oriented programming), Genome-wide association study, Parkinson Disease, Computational biology, Tag SNP, Biology, Signal, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Article, Apolipoproteins E, Gene Frequency, alpha-Synuclein, Humans, Genetic Predisposition to Disease, Genetics (clinical), Genetic association, Common disease-common variant, Genome-Wide Association Study

Abstract

In recent years, genome-wide association studies have been very successful in identifying loci for complex traits. However, typically these findings involve noncoding and/or intergenic SNPs without a clear functional effect that do not directly point to a gene. Hence, the challenge is to identify the causal variant responsible for the association signal. Typically, the first step is to identify all genetic variation in the locus region, usually by resequencing a large number of case chromosomes. Among all variants, the causal one needs to be identified in further functional studies. Because the experimental follow up can be very laborious, restricting the number of variants to be scrutinized can yield a great advantage. An objective method for choosing the size of the region to be followed up would be highly valuable. Here, we propose a simple method to call the minimal region around a significant association peak that is very likely to contain the causal variant. We model linkage disequilibrium (LD) in cases from the observed single SNP association signals, and predict the location of the causal variant by quantifying how well this relationship fits the data. Simulations showed that our approach identifies genomic regions of on average ∼50 kb with up to 90% probability to contain the causal variant. We apply our method to two genome-wide association data sets and localize both the functional variant REP1 in the synuclein gene that conveys susceptibility to Parkinson's disease and the APOE gene responsible for the association signal in the Alzheimer's disease data set. © 2014 Macmillan Publishers Limited All rights reserved.

Published

2014

10. Estimating and testing linkage disequilibrium from sib data

Author

Zoltán Bochdanovits, Dorret I. Boomsma, Aad van der Vaart, and Marianne A. Jonker

Subjects

Statistics and Probability, Linkage disequilibrium, Likelihood-ratio test, Statistics, Haplotype, Expectation–maximization algorithm, Estimator, Statistics, Probability and Uncertainty, Twin study, Dizygotic twins, Mathematics, Recombination Fraction

Abstract

We consider estimation and testing of linkage equilibrium from genotypic data on a random sample of sibs, such as monozygotic and dizygotic twins. We compute the maximum likelihood estimator with an EM-algorithm and a likelihood ratio statistic that takes the family structure into account. As we are interested in applying this to twin data we also allow observations on single children, so that monozygotic twins can be included. We allow non-zero recombination fraction between the loci of interest, so that linkage disequilibrium between both linked and unlinked loci can be tested. The EM-algorithm for computing the maximum likelihood estimator of the haplotype frequencies and the likelihood ratio test-statistic, are described in detail. It is shown that the usual estimators of haplotype frequencies based on ignoring that the sibs are related are inefficient, and the likelihood ratio test for testing that the loci are in linkage disequilibrium. © 2011 The Authors. Statistica Neerlandica © 2011 VVS.

Published

2011

11. The Role of the Brain-Derived Neurotrophic Factor (BDNF) val66met Variant in the Phenotypic Expression of Obsessive-Compulsive Disorder (OCD)

Author

Dan J. Stein, David Sondervan, Hilga Katerberg, Christine Lochner, Peter Heutink, Sian M. J. Hemmings, Danielle C. Cath, Paul D. Carey, J.A. den Boer, Zoltán Bochdanovits, A.J.L.M. van Balkom, de Peter Jonge, Annemiek Polman, Johanna C. Moolman-Smook, Science in Healthy Ageing & healthcaRE (SHARE), Interdisciplinary Centre Psychopathology and Emotion regulation (ICPE), Life Course Epidemiology (LCE), Human genetics, Psychiatry, and NCA - Anxiety & Depression

Subjects

Adult, Male, medicine.medical_specialty, Genotype, ANXIETY BEHAVIOR, Mutation, Missense, EARLY-ONSET, 5-HTTLPR, Severity of Illness Index, symptom dimensions, Cellular and Molecular Neuroscience, Young Adult, AFFECTED SIBLING PAIRS, Sex Factors, age of onset, Internal medicine, medicine, Humans, Family history, Obsessive-compulsive disorder (OCD), Genetics (clinical), Genetic Association Studies, Brain-derived neurotrophic factor, Family Health, Psychiatric Status Rating Scales, item-level factor analysis, LA-TOURETTE-SYNDROME, business.industry, Brain-Derived Neurotrophic Factor, Yale-Brown obsessive compulsive scale severity, ASSOCIATION, Middle Aged, SEROTONIN TRANSPORTER FUNCTION, medicine.disease, POLYMORPHISM, Genotype frequency, obsessive-compulsive disorder, COLLABORATIVE GENETICS, Psychiatry and Mental health, Endocrinology, Phenotype, Case-Control Studies, Female, Age of onset, business, Anxiety disorder

Abstract

Evidence suggests that the Va166Met variant of the brain-derived neurotrophic factor (BDNF) gene may play a role in the etiology of Obsessive-Compulsive Disorder (OCD). In this study, the role of the BDNF Va166Met variant in the etiology and the phenotypic expression of OCD is investigated. Associations between the BDNF Va166Met variant and OCD, obsessive-compulsive symptom dimensions, Yale-Brown Obsessive Compulsive Scale (YBOCS) severity scores, age of onset and family history of obsessive-compulsive symptoms were assessed. The BDNF Va166Met variant was genotyped in 419 patients with sub-/ clinical OCD and 650 controls. No differences in allele or genotype frequency were observed between cases and controls. In females with OCD, the Met66Met genotype was associated with later age of onset and a trend for a negative family history, whereas the Val66Val genotype was associated with a trend for lower YBOCS severity scores. Item-level factor analysis revealed six factors: 1) Contamination/cleaning; 2) Aggressive obsessions/checking; 3) Symmetry obsessions, counting, ordering and repeating; 4) Sexual/religious obsessions; 5) Hoarding and 6) Somatic obsessions/checking. A trend was found for a positive association between Factor 4 (Sexual/religious obsessions) and the BDNF Val66Val genotype. The results suggest that BDNF function may be implicated in the mediation of OCD. We found that for the BDNF Met66Met genotype may be associated with a milder phenotype in females and a possible role for the BDNF Val66Val genotype and the BDNF Val66 allele in the sexual/religious obsessions. (C) 2009 Wiley-Liss, Inc.

Published

2009

12. Global similarity with local differences in linkage disequilibrium between the Dutch and HapMap–CEU populations

Author

Patrick F. Sullivan, Luba M. Pardo, Brenda W.J.H. Penninx, Jouke J. Hottenga, Peter Heutink, Zoltán Bochdanovits, Danielle Posthuma, Eco J. C. de Geus, Dorret I. Boomsma, Human genetics, Psychiatry, NCA - Anxiety & Depression, Biological Psychology, and Neuroscience Campus Amsterdam - Anxiety & Depression

Subjects

HAPLOTYPE BLOCKS, Netherlands Twin Register (NTR), Linkage disequilibrium, Dutch population, INFORMATION, Genotype, Population, GENETIC-ASSOCIATION, Genome-wide association study, Single-nucleotide polymorphism, Biology, Population stratification, Polymorphism, Single Nucleotide, HapMap-CEU, Article, Linkage Disequilibrium, White People, 03 medical and health sciences, Gene Frequency, Genetics, Humans, natural sciences, International HapMap Project, GENOME-WIDE ASSOCIATION, WORLDWIDE SURVEY, education, Genetics (clinical), 030304 developmental biology, Genetic association, pair-wise LD, Netherlands, Linkage (software), 0303 health sciences, education.field_of_study, SNP DATA, COMPLEX TRAITS, 030305 genetics & heredity, TAGSNP TRANSFERABILITY, Genetics, Population, Evolutionary biology, SAMPLE-SIZE, PATTERNS, bootstrapping, LD blocks, Genome-Wide Association Study

Abstract

The HapMap project has facilitated the selection of tagging single nucleotide polymorphisms (tagSNPs) for genome-wide association studies (GWAS) under the assumption that linkage disequilibrium (LD) in the HapMap populations is similar to the populations under investigation. Earlier reports support this assumption, although in most of these studies only a few loci were evaluated. We compared pair-wise LD and LD block structure across autosomes between the Dutch population and the CEU-HapMap reference panel. The impact of sampling distribution on the estimation of LD blocks was studied by bootstrapping. A high Pearson correlation (genome-wide; 0.93) between pair-wise r(2) for the Dutch and the CEU populations was found, indicating that tagSNPs from the CEU-HapMap panel capture common variation in the Dutch population. However, some genomic regions exhibited, significantly lower correlation than the genome-wide estimate. This might decrease the validity of HapMap tagSNPs in these regions and the power of GWAS. The LD block structure differed considerably between the Dutch and CEU-HapMap populations. This was not explained by demographic differences between the CEU and Dutch samples, as testing for population stratification was not significant. We also found that sampling variation had a large effect on the estimation of LD blocks, as shown by the bootstrapping analysis. Thus, in small samples, most of the observed differences in LD blocks between populations are most likely the result of sampling variation. This poor concordance in LD block structure suggests that large samples are required for robust estimations of local LD block structure in populations. European Journal of Human Genetics (2009) 17, 802-810; doi: 10.1038/ejhg.2008.248; published online 7 January 2009

Published

2009

13. Determining the genome-wide kinship coefficient seems unhelpful in distinguishing consanguineous couples with a high versus low risk for adverse reproductive outcome

Author

Peter Heutink, Fowzan S. Alkuraya, Eamonn Sheridan, Lidewij Henneman, Martina C. Cornel, Piet J. Kostense, A. van Haeringen, Patrizia Rizzu, Wided Kelmemi, Jan-Maarten Cobben, Amira Masri, M. Hashem, Hülya Kayserili, Zoltán Bochdanovits, Charlotte J. Dommering, Sander Ouburg, Marieke Teeuw, Marianne A. Jonker, L. P. ten Kate, H. Bouhamed-Chaabouni, Complex Trait Genetics, Neuroscience Campus Amsterdam - Neurobiology of Mental Health, EMGO+ - Quality of Care, Neuroscience Campus Amsterdam - Brain Mechanisms in Health & Disease, Amsterdam Neuroscience, Other Research, Human Genetics, Paediatric Genetics, Human genetics, Medical Microbiology and Infection Prevention, Epidemiology and Data Science, NCA - Brain mechanisms in health and disease, NCA - Neurobiology of mental health, EMGO - Quality of care, Karabey, Hülya Kayserili (ORCID 0000-0003-0376-499X & YÖK ID 7945), Kelmemi, W., Teeuw, M. W., Bochdanovits, Z., Ouburg, S., Jonker, M. A., Alkuraya, F., Hashem, M., Kayserili, H., Haeringen, van A., Sheridan, E., Masri, A., Cobben, J. M., Rizzu, P., Kostense, P. J., Dommering, C. J., Henneman, L., Bouhamed-Chaabouni, H., Heutink, P., Cornel, L. P. ten Kate and M. C., School of Medicine, and Department of Medical Genetics

Subjects

Male, Linkage disequilibrium, Genotype, genetics [Congenital Abnormalities], Population, Inbreeding coefficient, Single-nucleotide polymorphism, Genes, Recessive, Consanguinity, Biology, Relatedness, Autosomal recessive disorder, Polymorphism, Single Nucleotide, Statistics, Nonparametric, Congenital Abnormalities, 03 medical and health sciences, Kinship, Genetics, Humans, Genetics(clinical), ddc:610, genetics [Genome, Human], education, Genetics (clinical), 030304 developmental biology, 0303 health sciences, education.field_of_study, Base Sequence, Genome, Human, Medical genetics, 030305 genetics & heredity, Case-control study, Regression analysis, Sequence Analysis, DNA, Pedigree, Case-Control Studies, Mann–Whitney U test, Female, Research Article

Abstract

Offspring of consanguineous couples are at increased risk of congenital disorders. The risk increases as parents are more closely related. Individuals that have the same degree of relatedness according to their pedigree, show variable genomic kinship coefficients. To investigate whether we can differentiate between couples with high- and low risk for offspring with congenital disorders, we have compared the genomic kinship coefficient of consanguineous parents with a child affected with an autosomal recessive disorder with that of consanguineous parents with only healthy children, corrected for the degree of pedigree relatedness. 151 consanguineous couples (73 cases and 78 controls) from 10 different ethnic backgrounds were genotyped on the Affymetrix platform and passed quality control checks. After pruning SNPs in linkage disequilibrium, 57,358 SNPs remained. Kinship coefficients were calculated using three different toolsets: PLINK, King and IBDelphi, yielding five different estimates (IBDelphi, PLINK (all), PLINK (by population), King robust (all) and King homo (by population)). We performed a one-sided Mann Whitney test to investigate whether the median relative difference regarding observed and expected kinship coefficients is bigger for cases than for controls. Furthermore, we fitted a mixed effects linear model to correct for a possible population effect. Although the estimated degrees of genomic relatedness with the different toolsets show substantial variability, correlation measures between the different estimators demonstrated moderate to strong correlations. Controls have higher point estimates for genomic kinship coefficients. The one-sided Mann Whitney test did not show any evidence for a higher median relative difference for cases compared to controls. Neither did the regression analysis exhibit a positive association between case–control status and genomic kinship coefficient. In this case–control setting, in which we compared consanguineous couples corrected for degree of pedigree relatedness, a higher degree of genomic relatedness was not significantly associated with a higher likelihood of having an affected child. Further translational research should focus on which parts of the genome and which pathogenic mutations couples are sharing. Looking at relatedness coefficients by determining genome-wide SNPs does not seem to be an effective measure for prospective risk assessment in consanguineous parents., NA

Published

2015

14. Latitudinal clines inDrosophila melanogaster: Body size, allozyme frequencies, inversion frequencies, and the insulin-signalling pathway

Author

Gerdien de Jong and Zoltán Bochdanovits

Subjects

Genetics, Reproductive success, Climate, Genetic Variation, Biology, biology.organism_classification, Drosophila melanogaster, Chromosome regions, Chromosome Inversion, Genetic variation, Genotype, Melanogaster, Animals, Body Constitution, Insulin, Allele frequency, Signal Transduction, Chromosomal inversion

Abstract

Many latitudinal clines exist in Drosophila melanogaster: in adult body size, in allele frequency at allozyme loci, and in frequencies of common cosmopolitan inversions. The question is raised whether these latitudinal clines are causally related. This review aims to connect data from two very different fields of study, evolutionary biology and cell biology, in explaining such natural genetic variation in D. melanogaster body size and development time. It is argued that adult body size clines, inversion frequency clines, and clines in allele frequency at loci involved in glycolysis and glycogen storage are part of the same adaptive strategy. Selection pressure is expected to differ at opposite ends of the clines. At high latitudes, selection on D. melanogaster would favour high larval growth rate at low temperatures, and resource storage in adults to survive winter. At low latitudes selection would favour lower larval critical size to survive crowding, and increased male activity leading to high male reproductive success. Studies of the insulin-signalling pathway in D. melanogaster point to the involvement of this pathway in metabolism and adult body size. The genes involved in the insulin-signalling pathway are associated with common cosmopolitan inversions that show latitudinal clines. Each chromosome region connected with a large common cosmopolitan inversion possesses a gene of the insulin transmembrane complex, a gene of the intermediate pathway and a gene of the TOR branch. The hypothesis is presented that temperate D. melanogaster populations have a higher frequency of a 'thrifty' genotype corresponding to high insulin level or high signal level, while tropical populations possess a more 'spendthrift' genotype corresponding to low insulin or low signal level.

Published

2003

15. Temperature dependence of fitness components in geographical populations of Drosophila melanogaster: changing the association between size and fitness

Author

Zoltán Bochdanovits and Gerdien de Jong

Subjects

education.field_of_study, Population fragmentation, Natural selection, Population, Biology, biology.organism_classification, Genetic load, Life history theory, Evolutionary biology, Drosophila melanogaster, Adaptation, education, Ecology, Evolution, Behavior and Systematics, Selection (genetic algorithm)

Abstract

Contrary to the conventional wisdom ‘bigger is better’, evolution at high temperature invariably leads to small individuals in Drosophila melanogaster. Natural selection is known to be responsible, meaning that genotypes that are small because of adaptation to high temperature must have some temperature dependent fitness advantage. In this study we consider both preadult and adult fitness components, and show that large adults from a cold adapted population significantly outperform small adults from a warm adapted population only when tested at low temperature and low larval density. In all other conditions ‘bigger is not necessarily better’, meaning that environmental influences are capable of altering the association between size and fitness. Yet, ‘smaller wasn’t better either’ under any condition, when considering the overall measure of fitness. Examination of individual fitness components revealed population by temperature interaction in preadult survival; this interaction is potentially capable of explaining the temperature specific advantage of small adult body size. At high temperature, the warm adapted population exhibits superior preadult survival while producing small adults. Geographical variation in adult body size seems to be the result of selection on larval growth and competitive strategies, resulting in alterations in the association between fitness components. © 2003 The Linnean Society of London, Biological Journal of the Linnean Society, 2003, 80, 717–725.

Published

2003

16. Covariation of Larval Gene Expression and Adult Body Size in Natural Populations of Drosophila melanogaster

Author

Zoltán Bochdanovits, Herman van der Klis, and Gerdien de Jong

Subjects

Quantitative Trait Loci, Gene Expression, Quantitative trait locus, Evolution, Molecular, Genetic variation, Gene expression, Genetics, Animals, RNA, Messenger, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, Oligonucleotide Array Sequence Analysis, biology, Metamorphosis, Biological, Temperature, Gene Expression Regulation, Developmental, Genetic Variation, biology.organism_classification, Phenotype, Drosophila melanogaster, Body Constitution, Developmental plasticity, Female, Adaptation

Abstract

Understanding adaptive phenotypic variation is one of the most fundamental problems in evolutionary biology. Genes involved in adaptation are most likely those that affect traits most intimately connected to fitness: life-history traits. The genetics of quantitative trait variation (including life histories) is still poorly understood, but several studies suggest that (1) quantitative variation might be the result of variation in gene expression, rather than protein evolution, and (2) natural variation in gene expression underlies adaptation. The next step in studying the genetics of adaptive phenotypic variation is therefore an analysis of naturally occuring covariation of global gene expression and a life-history trait. Here, we report a microarray study addressing the covariation in larval gene expression and adult body weight, a life-history trait involved in adaptation. Natural populations of Drosophila melanogaster show adaptive geographic variation in adult body size, with larger animals at higher latitudes. Conditions during larval development also affect adult size with larger flies emerging at lower temperatures. We found statistically significant differences in normalized larval gene expression between geographic populations at one temperature (genetic variation) and within geographic populations between temperatures (developmental plasticity). Moreover, larval gene expression correlated highly with adult weight, explaining 81% of its natural variation. Of the genes that show a correlation of gene expression with adult weight, most are involved in cell growth or cell maintenance or are associated with growth pathways.

Published

2003

17. Joint reanalysis of 29 correlated SNPs supports the role of PCLO/Piccolo as a causal risk factor for major depressive disorder

Author

August B. Smit, B.W.J.H. Penninx, Peter Heutink, E.J.C. de Geus, Danielle Posthuma, Zoltán Bochdanovits, Dorret I. Boomsma, Matthijs Verhage, Witte J.G. Hoogendijk, Human genetics, Psychiatry, NCA - Anxiety & Depression, Functional Genomics, Molecular and Cellular Neurobiology, Biological Psychology, and Neuroscience Campus Amsterdam - Anxiety & Depression

Subjects

Genetics, Netherlands Twin Register (NTR), Depressive Disorder, Major, Neuropeptides, Single-nucleotide polymorphism, medicine.disease, Polymorphism, Single Nucleotide, Cytoskeletal Proteins, Cellular and Molecular Neuroscience, Psychiatry and Mental health, Risk Factors, medicine, Humans, Major depressive disorder, Genetic Predisposition to Disease, Risk factor, Psychology, Molecular Biology, Genome-Wide Association Study, Probability

Abstract

Joint reanalysis of 29 correlated SNPs supports the role of PCLO/ Piccolo as a causal risk factor for major depressive disorder

Published

2009

18. Resequencing Three Candidate Genes for Major Depressive Disorder in a Dutch Cohort

Author

Marianna R. Bevova, Zoltán Bochdanovits, Tiny Uithuisje, Johannes H. Smit, I. Bakker, Eva C. Verbeek, Patrizia Rizzu, Eco J. C. de Geus, Brenda W.J.H. Penninx, Dorret I. Boomsma, Witte J.G. Hoogendijk, Peter Heutink, Functional Genomics, Biological Psychology, Neuroscience Campus Amsterdam - Brain Mechanisms in Health & Disease, Neuroscience Campus Amsterdam - Neurobiology of Mental Health, EMGO+ - Mental Health, Neuroscience Campus Amsterdam - Brain Imaging Technology, Clinical Genetics, Psychiatry, Human genetics, Epidemiology and Data Science, NCA - Brain mechanisms in health and disease, NCA - Neurobiology of mental health, EMGO - Mental health, and NCA - Brain imaging technology

Subjects

Netherlands Twin Register (NTR), Linkage disequilibrium, Candidate gene, lcsh:Medicine, Single-nucleotide polymorphism, Genome-wide association study, Biology, Receptors, Metabotropic Glutamate, Polymorphism, Single Nucleotide, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, mental disorders, SNP, Humans, lcsh:Science, Promoter Regions, Genetic, 030304 developmental biology, Genetic association, Netherlands, Genetics, Serotonin Plasma Membrane Transport Proteins, 0303 health sciences, Depressive Disorder, Major, Multidisciplinary, lcsh:R, Neuropeptides, Epistasis, Genetic, Cytoskeletal Proteins, Haplotypes, Cohort, lcsh:Q, 030217 neurology & neurosurgery, Imputation (genetics), Research Article, Genome-Wide Association Study

Abstract

Major depressive disorder (MDD) is a psychiatric disorder, characterized by periods of low mood of more than two weeks, loss of interest in normally enjoyable activities and behavioral changes. MDD is a complex disorder and does not have a single genetic cause. In 2009 a genome wide association study (GWAS) was performed on the Dutch GAIN-MDD cohort. Many of the top signals of this GWAS mapped to a region spanning the gene PCLO, and the non-synonymous coding single nucleotide polymorphism (SNP) rs2522833 in the PCLO gene became genome wide significant after post-hoc analysis. We performed resequencing of PCLO, GRM7, and SLC6A4 in 50 control samples from the GAIN-MDD cohort, to detect new genomic variants. Subsequently, we genotyped these variants in the entire GAIN-MDD cohort and performed association analysis to investigate if rs2522833 is the causal variant or simply in linkage disequilibrium with a more associated variant. GRM7 and SLC6A4 are both candidate genes for MDD from literature. We aimed to gather more evidence that rs2522833 is indeed the causal variant in the GAIN-MDD cohort or to find a previously undetected common variant in either PCLO, GRM7, or SLC6A4 with a higher association in this cohort. After next generation sequencing and association analysis we excluded the possibility of an undetected common variant to be more associated. For neither PCLO nor GRM7 we found a more associated variant. For SLC6A4, we found a new SNP that showed a lower P-value (P = 0.07) than in the GAIN-MDD GWAS (P = 0.09). However, no evidence for genome-wide significance was found. Although we did not take into account rare variants, we conclude that our results provide further support for the hypothesis that the non-synonymous coding SNP rs2522833 in the PCLO gene is indeed likely to be the causal variant in the GAIN-MDD cohort. © 2013 Verbeek et al.

Published

2013

19. Cervical dystonia and genetic common variation in the dopamine pathway

Author

Majid Aramideh, Bart P.C. van de Warrenburg, Frank Baas, Peter Heutink, Jacobus J. van Hilten, Marina A. J. Tijssen, Justus L. Groen, Javier Simón-Sánchez, Zoltán Bochdanovits, Y. Fang, Agnita J.W. Boon, Katja Ritz, ANS - Amsterdam Neuroscience, Pathology, Genome Analysis, Other departments, Human genetics, NCA - Brain mechanisms in health and disease, NCA - neurodegeneration, Functional Genomics, Neuroscience Campus Amsterdam - Neurodegeneration, and Neuroscience Campus Amsterdam - Brain Mechanisms in Health & Disease

Subjects

Male, Genotype, Dopamine, DCN MP - Plasticity and memory, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, SDG 3 - Good Health and Well-being, Genetic variation, medicine, Humans, Genetic Predisposition to Disease, Cervical dystonia, Polymorphism, Dopamine pathway, Torticollis, Netherlands, Dystonia, Genetics, Common variants, Haplotype, Genetic Variation, Single Nucleotide, Focal dystonia, Middle Aged, medicine.disease, Neurology, Female, Neurology (clinical), Geriatrics and Gerontology, medicine.drug

Abstract

Cervical dystonia, a late onset focal dystonia, has a complex genetic background. Multiple lines of evidence point to a role for aberrant dopamine levels in dystonia. We assessed whether common variation within genes that regulate brain dopamine levels and in key genes of the dopamine metabolic pathway, modulate the risk for cervical dystonia. DNA was collected from 363 Dutch CD patients and a cohort of Dutch control individuals. Haplotype-tagging single nucleotide polymorphisms (SNPs) complemented with selected variants of functional importance in COMT, DAT, TH, MAO-A and -B, DDC and DBH were investigated. We tested the 143 markers in single-SNP, haplotype and epistasis analyses. We did not find an association with any of the selected 143 SNPs in these key dopamine genes. Our data shows that common variations in key genes of the dopamine pathway do not contribute to dystonia risk in the Dutch population. Possibly, risk alleles in this pathway may be rarer than detectable in this study, or might be located in downstream dopamine signaling pathway. Alternatively, found dopamine level changes are secondary to the dystonia disease processes. (C) 2012 Published by Elsevier Ltd

Published

2013

20. Piccolo genotype modulates neural correlates of emotion processing but not executive functioning

Author

D.J. Veltman, Brenda W.J.H. Penninx, M.A. van Buchem, Zoltán Bochdanovits, M-J van Tol, Saskia Woudstra, Frans G. Zitman, N.J. van der Wee, Liliana Ramona Demenescu, Esther M. Opmeer, Witte J.G. Hoogendijk, André Aleman, Psychiatry, Human genetics, Anatomy and neurosciences, NCA - Anxiety & Depression, EMGO - Mental health, Interdisciplinary Centre Psychopathology and Emotion regulation (ICPE), Perceptual and Cognitive Neuroscience (PCN), Erasmus MC other, Neuroscience Campus Amsterdam - Anxiety & Depression, and EMGO+ - Mental Health

Subjects

Male, Neural substrate, Emotions, PCLO, FACES, Synaptic Transmission, Developmental psychology, AFFECTIVE FACIAL STIMULI, EXPRESSIONS, Monoaminergic, LONDON TASK, Serotonin transporter, MAJOR DEPRESSIVE DISORDER, medicine.diagnostic_test, biology, Genetic Carrier Screening, Cognition, Middle Aged, Amygdala, Magnetic Resonance Imaging, neuroimaging genetics, Facial Expression, Psychiatry and Mental health, medicine.anatomical_structure, Pattern Recognition, Visual, AMYGDALA ACTIVITY, Major depressive disorder, Original Article, Female, Psychology, Adult, MOOD DISORDERS, Genotype, behavioral disciplines and activities, Cellular and Molecular Neuroscience, ANTIDEPRESSANT TREATMENT, Image Interpretation, Computer-Assisted, medicine, Humans, Genetic Predisposition to Disease, Dominance, Cerebral, Biological Psychiatry, Alleles, Depressive Disorder, Major, Polymorphism, Genetic, emotion processing, Neuropeptides, medicine.disease, Image Enhancement, Oxygen, Cytoskeletal Proteins, executive function, SEROTONIN TRANSPORTER, biology.protein, genome-wide association, Functional magnetic resonance imaging, Neuroscience, Executive dysfunction, Genome-Wide Association Study

Abstract

Translational psychiatry 2012(2), e99 (2012). doi:10.1038/tp.2012.29, Published by Nature Publishing Group, London

Published

2012

21. Extended Kindred With Recessive Late-Onset Alzheimer Disease Maps to Locus 8p22-p21.2 A Genome-wide Linkage Analysis

Author

Adriano Jimenez-Escrig, Alberto Rábano, Zoltán Bochdanovits, Isabel Gobernado, Peter Heutink, David G. Munoz, Manuel Baron, Estrella Gómez-Tortosa, Human genetics, NCA - Neurodegeneration, and Neuroscience Campus Amsterdam - Neurodegeneration

Subjects

Male, Candidate gene, Genotype, Genetic Linkage, Population, Single-nucleotide polymorphism, Locus (genetics), Genes, Recessive, Biology, Polymorphism, Single Nucleotide, Apolipoproteins E, Alzheimer Disease, medicine, Humans, Genetic Predisposition to Disease, Age of Onset, education, Gene, Genotyping, Genetics, education.field_of_study, Genome, Genetic disorder, Chromosome Mapping, medicine.disease, Pedigree, Psychiatry and Mental health, Clinical Psychology, Genetic Loci, Female, Geriatrics and Gerontology, Lod Score, Gerontology, Inbreeding, Chromosomes, Human, Pair 8, Genome-Wide Association Study

Abstract

Late-onset Alzheimer disease (LOAD) is a complex genetic disorder. Although genes involved in early-onset forms were discovered more than a decade ago, LOAD research has only been able to point out small effect loci, with the exception of APOE. We mapped the gene predisposing to LOAD in an extended inbred family coming from a genetically isolated region (24 sampled individuals, 12 of whom are affected), completing a genome-wide screen with an Affymetrix10 K single nucleotide polymorphism microarray. Genotyping results were evaluated under model-dependent (dominant and recessive) and model-free analysis. We obtained a maximum nonparametric linkage score of 3.24 (P=0.00006) on chromosome 8p22-p21.2. The same genomic position also yielded the highest multipoint heterogeneity LOD (HLOD) under a recessive model (HLOD=3.04). When we compared the results of the model-dependent analysis, a higher score was obtained in the recessive model (3.04) than in the dominant model (1.0). This is a new locus identified in LOAD, in chromosome 8p22-p21.2 and encompassing several candidate genes, among them CLU and PPP3CC that were excluded by sequencing. The finding of a recessive model of inheritance, consistent with the assumption of inbreeding as a morbidity factor in this population, supports the notion of a role of recessive genes in LOAD. Copyright © 2012 by Lippincott Williams & Wilkins.

Published

2012

22. Genome-wide association study confirms extant PD risk loci among the Dutch

Author

Sampath Arepalli, Zoltán Bochdanovits, Rob M.A. de Bie, Bart P.C. van de Warrenburg, Albert Hofman, Bart Post, Peter Heutink, Fernando Rivadeneira, Andrew B. Singleton, Dena G. Hernandez, Hans Scheffer, Jacobus J. van Hilten, Karin van Dijk, B.R. Bloem, Daan C. Velseboer, Henk W. Berendse, Patrizia Rizzu, André G. Uitterlinden, Javier Simón-Sánchez, Erasmus MC other, Internal Medicine, Epidemiology, Clinical Genetics, Human genetics, Neurology, Anatomy and neurosciences, NCA - Neurodegeneration, Neuroscience Campus Amsterdam - Neurodegeneration, ANS - Amsterdam Neuroscience, ACS - Amsterdam Cardiovascular Sciences, and Graduate School

Subjects

Male, Linkage disequilibrium, Genome-wide association study, Genomic disorders and inherited multi-system disorders Functional Neurogenomics [IGMD 3], 0302 clinical medicine, Gene Frequency, Risk Factors, Genotype, MAPT, Age of Onset, Genetics (clinical), Netherlands, Aged, 80 and over, Genetics, 0303 health sciences, Intracellular Signaling Peptides and Proteins, Parkinson Disease, Middle Aged, HLA, alpha-Synuclein, PD, Female, Functional Neurogenomics [DCN 2], Adult, Adolescent, BST1, tau Proteins, Single-nucleotide polymorphism, Locus (genetics), Human leukocyte antigen, Protein Serine-Threonine Kinases, Biology, GPI-Linked Proteins, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Antigens, CD, Humans, Genetic Predisposition to Disease, GAK/DGKQ, ADP-ribosyl Cyclase, Allele frequency, Aged, 030304 developmental biology, Case-control study, DNA Fingerprinting, Genetic Loci, Case-Control Studies, SNCA, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

In view of the population-specific heterogeneity in reported genetic risk factors for Parkinson's disease (PD), we conducted a genome-wide association study (GWAS) in a large sample of PD cases and controls from the Netherlands. After quality control (QC), a total of 514 799 SNPs genotyped in 772 PD cases and 2024 controls were included in our analyses. Direct replication of SNPs within SNCA and BST1 confirmed these two genes to be associated with PD in the Netherlands (SNCA, rs2736990: P=1.63x10(-5), OR=1.325 and BST1, rs12502586: P=1.63x10(-3), OR=1.337). Within SNCA, two independent signals in two different linkage disequilibrium (LD) blocks in the 3' and 5' ends of the gene were detected. Besides, post-hoc analysis confirmed GAK/DGKQ, HLA and MAPT as PD risk loci among the Dutch (GAK/DGKQ, rs2242235: P=1.22x10(-4), OR=1.51; HLA, rs4248166: P=4.39x10(-5), OR=1.36; and MAPT, rs3785880: P=1.9x10(-3), OR=1.19). European Journal of Human Genetics (2011) 19, 655-661; doi:10.1038/ejhg.2010.254; published online 19 January 2011

Published

2011

23. The Complete Automation of Cell Culture: Improvements for High-Throughput and High-Content Screening

Author

David Sondervan, Daniel Caminada, Zoltán Bochdanovits, Peter Heutink, Shushant Jain, Patrizia Rizzu, Human genetics, NCA - Drug Screening & Therapy Design, and Neuroscience Campus Amsterdam - Drug Screening & Therapy Design

Subjects

Cell Survival, Cell Culture Techniques, Nanotechnology, Computational biology, Biology, Biochemistry, Cell Line, Analytical Chemistry, Mammalian cell, High-Throughput Screening Assays, Humans, Throughput (business), Cell survival, Automation, Laboratory, business.industry, Reproducibility of Results, Genomics, Automation, Molecular Imaging, Identification (information), Cell culture, High-content screening, Molecular Medicine, RNA Interference, business, Software, Biotechnology

Abstract

Genomic approaches provide enormous amounts of raw data with regard to genetic variation, the diversity of RNA species, and protein complement. high-throughput (HT) and high-content (HC) cellular screens are ideally suited to contextualize the information gathered from other "omic" approaches into networks and can be used for the identification of therapeutic targets. Current methods used for HT-HC screens are laborious, time-consuming, and prone to human error. The authors thus developed an automated high-throughput system with an integrated fluorescent imager for HC screens called the AI. CELLHOST. The implementation of user-defined culturing and assay plate setup parameters allows parallel operation of multiple screens in diverse mammalian cell types. The authors demonstrate that such a system is able to successfully maintain different cell lines in culture for extended periods of time as well as significantly increasing throughput, accuracy, and reproducibility of HT and HC screens. © 2011 Society for Laboratory Automation and Screening.

Published

2011

24. Do consanguineous parents of a child affected by an autosomal recessive disease have more DNA identical-by-descent than similarly-related parents with healthy offspring? Design of a case-control study

Author

Peter Heutink, Zoltán Bochdanovits, Leo P. ten Kate, Martina C. Cornel, Marieke Teeuw, D.J. Kuik, Lidewij Henneman, Human genetics, Epidemiology and Data Science, EMGO - Quality of care, NCA - Integrative Analysis & Modeling, Neuroscience Campus Amsterdam - integrative Analysis & Modeling, and EMGO+ - Quality of Care

Subjects

Male, Parents, lcsh:Internal medicine, lcsh:QH426-470, Offspring, Chromosome Disorders, Genes, Recessive, Consanguinity, Ethnic origin, Disease, Identity by descent, Risk Assessment, Study Protocol, SDG 3 - Good Health and Well-being, Reference Values, Genetic variation, Prevalence, Genetics, Medicine, Humans, Genetics(clinical), lcsh:RC31-1245, Child, Genetics (clinical), Stochastic Processes, business.industry, Case-control study, Genetic Variation, DNA, Pedigree, lcsh:Genetics, Female, business, Risk assessment, Demography

Abstract

Background The offspring of consanguineous relations have an increased risk of congenital/genetic disorders and early mortality. Consanguineous couples and their offspring account for approximately 10% of the global population. The increased risk for congenital/genetic disorders is most marked for autosomal recessive disorders and depends on the degree of relatedness of the parents. For children of first cousins the increased risk is 2-4%. For individual couples, however, the extra risk can vary from zero to 25% or higher, with only a minority of these couples having an increased risk of at least 25%. It is currently not possible to differentiate between high-and low-risk couples. The quantity of DNA identical-by-descent between couples with the same degree of relatedness shows a remarkable variation. Here we hypothesize that consanguineous partners with children affected by an autosomal recessive disease have more DNA identical-by-descent than similarly-related partners who have only healthy children. The aim of the study is thus to establish whether the amount of DNA identical-by-descent in consanguineous parents of children with an autosomal recessive disease is indeed different from its proportion in consanguineous parents who have healthy children only. Methods/Design This project is designed as a case-control study. Cases are defined as consanguineous couples with one or more children with an autosomal recessive disorder and controls as consanguineous couples with at least three healthy children and no affected child. We aim to include 100 case couples and 100 control couples. Control couples are matched by restricting the search to the same family, clan or ethnic origin as the case couple. Genome-wide SNP arrays will be used to test our hypothesis. Discussion This study contains a new approach to risk assessment in consanguineous couples. There is no previous study on the amount of DNA identical-by-descent in consanguineous parents of affected children compared to the consanguineous parents of healthy children. If our hypothesis proves to be correct, further studies are needed to obtain different risk figure estimates for the different proportions of DNA identical-by-descent. With more precise information about their risk status, empowerment of couples can be improved when making reproductive decisions.

Published

2010

25. The Role of the COMT Val(158)Met Polymorphism in the Phenotypic Expression of Obsessive-Compulsive Disorder

Author

Anton J.L.M. van Balkom, Peter Heutink, Filip Van Nieuwerburgh, Zoltán Bochdanovits, Danielle C. Cath, Damiaan Denys, Johan A. den Boer, Hilga Katerberg, Annemiek Polman, Dieter Deforce, Neuroscience Campus Amsterdam - Anxiety & Depression, EMGO+ - Mental Health, Human genetics, Psychiatry, NCA - Anxiety & Depression, EMGO - Mental health, and Adult Psychiatry

Subjects

Male, Obsessive-Compulsive Disorder, Candidate gene, Genotype, OC symptom severity, ANXIETY DISORDERS, INTERNATIONAL NEUROPSYCHIATRIC INTERVIEW, EARLY-ONSET, Single-nucleotide polymorphism, SUSCEPTIBILITY, Catechol O-Methyltransferase, behavioral disciplines and activities, SYMPTOM DIMENSIONS, Cellular and Molecular Neuroscience, Methionine, age of onset, O-METHYLTRANSFERASE COMT, DSM-IV, SDG 3 - Good Health and Well-being, mental disorders, LINKAGE, Humans, Medicine, Allele, Genetics (clinical), Genetics, Polymorphism, Genetic, Catechol-O-methyl transferase, OCD, business.industry, fungi, Valine, ASSOCIATION, medicine.disease, COMT, GENE, Twin study, humanities, OC symptom dimensions, Psychiatry and Mental health, Phenotype, Case-Control Studies, Female, Age of onset, Factor Analysis, Statistical, business, Anxiety disorder

Abstract

Obsessive-Compulsive Disorder (OCD) is characterized by the presence of obsessions and compulsions, and shows considerable phenotypic variability. Family and twin studies have indicated a genetic component in the etiology of OCD, and the catechol-O-methyl transferase (COMT) gene is an important candidate gene for OCD. This study investigates the influence of the functional COMT Val158Met polymorphism on the phenotypic expression of OCD, using an item-level factor-analytic approach in a large sample. The COMT Val158Met variant was genotyped in 373 patients and 462 controls. It was tested whether there was an association between the COMT Val158Met polymorphism and OCD or dimensional phenotypes such as YBOCS severity score, age of onset of obsessive-compulsive symptoms and six symptom dimensions recently found in a large item-level factor-analytic study [Katerberg et al., submitted]. We further investigated possible sex-specific associations between the COMT Val158Met polymorphism and OCD or dimensional phenotypes. There was a trend for an association of the COMT 158Met allele with OCD in males, and an interaction between the COMT Val158Met genotype and sex on the somatic and sensory phenomena symptom dimension, with females showing lower scores. In conclusion, a dimensional approach seems fruitful in detecting genes of importance for OCD. (C) 2009 Wiley-Liss, Inc.

Published

2010

26. Comprehensive mRNA expression profiling distinguishes tauopathies and identifies shared molecular pathways

Author

Zoltán Bochdanovits, Wouter Kamphorst, Peter Heutink, Rivka Ravid, Iraad F. Bronner, Patrizia Rizzu, John C. van Swieten, Human genetics, Pathology, NCA - Neurodegeneration, and Netherlands Institute for Neuroscience (NIN)

Subjects

Microarray, Gene regulatory network, lcsh:Medicine, Genome-wide association study, tau Proteins, Biology, Polymerase Chain Reaction, Progressive supranuclear palsy, medicine, Cluster Analysis, Humans, RNA, Messenger, lcsh:Science, Neurological Disorders/Movement Disorders, DNA Primers, Oligonucleotide Array Sequence Analysis, Genetics, Multidisciplinary, Gene Expression Profiling, lcsh:R, Neurodegenerative Diseases, Genetics and Genomics/Gene Expression, medicine.disease, Gene expression profiling, Neurological Disorders/Neurogenetics, Case-Control Studies, lcsh:Q, DNA microarray, Alzheimer's disease, Genetics and Genomics/Comparative Genomics, Neurological Disorders/Alzheimer Disease, Frontotemporal dementia, Genome-Wide Association Study, Research Article

Abstract

BACKGROUND:Understanding the aetiologies of neurodegenerative diseases such as Alzheimer's disease (AD), Pick's disease (PiD), Progressive Supranuclear Palsy (PSP) and Frontotemporal dementia (FTD) is often hampered by the considerable clinical and molecular overlap between these diseases and normal ageing. The development of high throughput genomic technologies such as microarrays provide a new molecular tool to gain insight in the complexity and relationships between diseases, as they provide data on the simultaneous activity of multiple genes, gene networks and cellular pathways. METHODOLOGY/PRINCIPAL FINDINGS:We have constructed genome wide expression profiles from snap frozen post-mortem tissue from the medial temporal lobe of patients with four neurodegenerative disorders (5 AD, 5 PSP, 5 PiD and 5 FTD patients) and 5 control subjects. All patients were matched for age, gender, ApoE-epsilon and MAPT (tau) haplotype. From all groups a total of 790 probes were shown to be differently expressed when compared to control individuals. The results from these experiments were then used to investigate the correlations between clinical, pathological and molecular findings. From the 790 identified probes we extracted a gene set of 166 probes whose expression could discriminate between these disorders and normal ageing. CONCLUSIONS/SIGNIFICANCE:From genome wide expression profiles we extracted a gene set of 166 probes whose expression could discriminate between neurological disorders and normal ageing. This gene set can be further developed into an accurate microarray-based classification test. Furthermore, from this dataset we extracted a disease specific set of genes and identified two aging related transcription factors (FOXO1A and FOXO3A) as possible drug targets related to neurodegenerative disease.

Published

2009

27. Variation at GRN 3 '-UTR rs5848 Is Not Associated with a Risk of Frontotemporal Lobar Degeneration in Dutch Population

Author

Peter Heutink, Dorly J. H. Deeg, Harro Seelaar, John C. van Swieten, Zoltán Bochdanovits, Javier Simón-Sánchez, Human genetics, Psychiatry, EMGO - Mental health, and NCA - Neurodegeneration

Subjects

Adult, Male, Risk, Genotype, Population, lcsh:Medicine, Single-nucleotide polymorphism, Biology, Genetics and Genomics/Complex Traits, Polymorphism, Single Nucleotide, Progranulins, Polymorphism (computer science), Genetic variation, Genetics and Genomics/Population Genetics, mental disorders, medicine, SNP, Dementia, Humans, education, lcsh:Science, 3' Untranslated Regions, Genetics and Genomics/Genetics of Disease, Aged, Netherlands, Genetics, Genetics and Genomics/Medical Genetics, education.field_of_study, Multidisciplinary, lcsh:R, Genetic Variation, nutritional and metabolic diseases, Frontotemporal lobar degeneration, Middle Aged, medicine.disease, nervous system diseases, DNA-Binding Proteins, Exact test, Intercellular Signaling Peptides and Proteins, Regression Analysis, Female, lcsh:Q, Frontotemporal Lobar Degeneration, Research Article

Abstract

Background: A single nucleotide polymorphism (rs5848) located in the 39- untranslated region of GRN has recently been associated with a risk of frontotemporal lobar degeneration (FTLD) in North American population particularly in pathologically confirmed cases with neural inclusions immunoreactive for ubiquitin and TAR DNA-binding protein 43 (TDP43), but negative for tau and alpha-synuclein (FTLD-TDP). Methodology/Principal Findings: In an effort to replicate these results in a different population, rs5848 was genotyped in 256 FTLD cases and 1695 controls from the Netherlands. Single SNP gender-adjusted logistic regression analysis revealed no significant association between variation at rs5848 and FTLD. Fisher’s exact test, failed to find any significant association between rs5848 and a subset of 23 pathology confirmed FTLD-TDP cases. Conclusions/Significance: The evidence presented here suggests that variation at rs5848 does not contribute to the etiology of FTLD in the Dutch population.

Published

2009

28. A functional polymorphism under positive evolutionary selection in ADRB2 is associated with human intelligence with opposite effects in the young and the elderly

Author

Dorret I. Boomsma, Linda M. van den Berg, Tinca J. C. Polderman, Michelle Luciano, Patrizia Rizzu, Zoltán Bochdanovits, John M. Starr, Peter Heutink, Sarah E. Harris, Ian J. Deary, Lorna M. Houlihan, Luba M. Pardo, Florencia M. Gosso, Eco J. C. de Geus, Danielle Posthuma, Biological Psychology, Neuroscience Campus Amsterdam - Attention & Cognition, Human genetics, and NCA - Attention & Cognition

Subjects

Adult, Male, Primates, Netherlands Twin Register (NTR), Candidate gene, Aging, Pan troglodytes, Population, Intelligence, Single-nucleotide polymorphism, Rodentia, Biology, Polymorphism, Single Nucleotide, Evolution, Molecular, Polymorphism (computer science), Genetics, Animals, Humans, Family, Allele, Selection, Genetic, education, Child, Gene, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Genetic association, Comparative genomics, education.field_of_study, Polymorphism, Genetic, Genome, Human, Brain, Proteins, Regression Analysis, Female, Receptors, Adrenergic, beta-2

Abstract

Comparative genomics offers a novel approach to unravel the genetic basis of complex traits. We performed a two stage analysis where genes ascertained for enhanced protein evolution in primates are subsequently searched for the presence of non-synonymous coding SNPs in the current human population at amino acid sites that differ between humans and chimpanzee. Positively selected genes among primates are generally presumed to determine phenotypic differences between humans and chimpanzee, such as the enhanced cognitive ability of our species. Amino acid substitutions segregating in humans at positively selected amino acid sites are expected to affect phenotypic differences among humans. Therefore we conducted an association study in two family based cohorts and one population based cohort between cognitive ability and the most likely candidate gene among the five that harbored more than one such polymorphism. The derived, human-specific allele of the beta-2 adrenergic receptor Arg16Gly polymorphism was found to be the increaser allele for performance IQ in the young, family based cohort but the decreaser allele for two different measures of cognition in the large Scottish cohort of unrelated individuals. The polymorphism is known to affect signaling activity and modulation of beta-2 adrenergic signaling has been shown to adjust memory consolidation, a trait related to cognition. The opposite effect of the polymorphism on cognition in the two age classes observed in the different cohorts resembles the effect of ADRB2 on hypertension, which also has been reported to be age dependent. This result illustrates the relevance of comparative genomics to detect genes that are involved in human behavior. © 2008 Springer Science+Business Media, LLC.

Published

2009

29. Adaptive differences in gene expression associated with heavy metal tolerance in the soil arthropod Orchesella cincta

Author

Dick Roelofs, Zoltán Bochdanovits, Thierry K. S. Janssens, Nico M. van Straalen, Benjamin Nota, M.J.T.N. Timmermans, Bauke Ylstra, Janine Mariën, Human genetics, Pathology, EMGO - Mental health, Animal Ecology, and EMGO+ - Mental Health

Subjects

DNA, Complementary, Evolution, Physiological, Population, Stress, Research Support, Evolution, Molecular, Soil, Stress, Physiological, Complementary, Gene expression, Genetics, Journal Article, Animals, Cluster Analysis, Soil Pollutants, Adaptation, education, Non-U.S. Gov't, Gene, Arthropods, Ecology, Evolution, Behavior and Systematics, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, education.field_of_study, biology, Abiotic stress, Research Support, Non-U.S. Gov't, Gene Expression Profiling, Molecular, Sequence Analysis, DNA, DNA, biology.organism_classification, Adaptation, Physiological, Gene expression profiling, Orchesella cincta, Gene Expression Regulation, Suppression subtractive hybridization, Sequence Analysis, Cadmium

Abstract

Field-selected tolerance to heavy metals has been reported for Orchesella cincta (Arthropoda: Collembola) populations occurring at metal-contaminated mining sites. This tolerance correlated with heritable increase in metal excretion efficiency, less pronounced cadmium (Cd)-induced growth reduction and overexpression of the metallothionein gene. We applied transcriptomics to determine differential gene expression caused by this abiotic stress in reference and Cd-tolerant populations. Many cDNAs responded to Cd exposure in the reference population. Significantly fewer clones were Cd responsive in tolerant animals. Analysis of variance revealed transcripts that interact between Cd exposure and population. Hierarchical cluster analysis of these clones identified two major groups. The first one contained cDNAs that were up-regulated by Cd in the reference culture but non-responsive or down-regulated in tolerant animals. This cluster was also characterized by elevated constitutive expression in the tolerant population. Gene ontology analysis revealed that these cDNAs were involved in structural integrity of the cuticle, anti-microbial defence, calcium channel-blocking, sulphur assimilation and chromatin remodelling. The second group consisted of cDNAs down-regulated in reference animals but not responding or slightly up-regulated in tolerant animals. Their functions involved carbohydrate metabolic processes, Ca(2+)-dependent stress signalling, redox state, proteolysis and digestion. The reference population showed a strong signature of stress-induced genome-wide perturbation of gene expression, whereas the tolerant animals maintained normal gene expression upon Cd exposure. We confirmed the micro-evolutionary processes occurring in soil arthropod populations and suggest a major contribution of gene regulation to the evolution of a stress-adapted phenotype.

Published

2009

30. Empirical assessment of the validity of the 'fundamental theorem of the HapMap' in the light of 'cryptic' tagging of multiple susceptibility loci

Author

Zoltán Bochdanovits, A. W. van der Vaart, Peter Heutink, Human genetics, Neuroscience Campus Amsterdam 2008, Stochastics, and Mathematics

Subjects

Genetics, Linkage disequilibrium, Linkage Disequilibrium Mapping, Haplotype, Chromosome Mapping, Reproducibility of Results, Locus (genetics), Genomics, Biology, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Bias, Haplotypes, Gene mapping, Sample size determination, Sample Size, Genetic Predisposition to Disease, International HapMap Project, Genetics (clinical), Genetic association

Abstract

Underestimation of the sample size needed to detect genetic association may occur as a result of deviations from the 'fundamental theorem of the HapMap'. A biologically plausible mechanism that might cause this deviation is 'cryptic' tagging of multiple susceptibility loci by the same neutral marker. For complex disorders, the existence of multiple susceptibility loci on the same chromosome is probably the rule rather than the exception. Our results show that conditional on the known haplotype structure of the genome the probability that a tagging SNP that is in linkage disequilibrium (LD) with a susceptibility gene is also in LD with another susceptibility gene is not negligible. Consequently, we were able to estimate the extent and the prevalence of the bias in the necessary sample size to find association induced by 'cryptic' tagging. In general, the underestimation of the necessary sample size is modest: 5% of all association studies will underestimate the sample size by 5-30%. On the basis of our results, a safe bet is to use a sample that is 10% larger than otherwise deemed necessary.

Published

2008

31. Genome-Wide Prediction of Functional Gene-Gene Interactions Inferred from Patterns of Genetic Differentiation in Mice and Men

Author

Sophie Perillous, David Sondervan, Zoltán Bochdanovits, Peter Heutink, Dorret I. Boomsma, Toos C. E. M. van Beijsterveldt, Biological Psychology, Neuroscience Campus Amsterdam 2008, and Human genetics

Subjects

Netherlands Twin Register (NTR), Candidate gene, Population, Population genetics, lcsh:Medicine, Genetics and Genomics/Complex Traits, Biology, Polymorphism, Single Nucleotide, Genome, Mice, 03 medical and health sciences, 0302 clinical medicine, Genetics and Genomics/Population Genetics, Methods, Animals, Humans, Gene Regulatory Networks, Evolutionary Biology/Genomics, education, lcsh:Science, Gene, 030304 developmental biology, Genetic association, Genetics, 0303 health sciences, education.field_of_study, Multidisciplinary, Genome, Human, lcsh:R, Computational Biology, Epistasis, Genetic, Genetics, Population, Evolutionary biology, Feasibility Studies, Epistasis, Human genome, lcsh:Q, 030217 neurology & neurosurgery, Research Article

Abstract

The human genome encodes a limited number of genes yet contribute to individual differences in a vast array of heritable traits. A possible explanation for the capacity our genome to generate this virtually unlimited range of phenotypic variation in complex traits to assume functional interactions between genes. Therefore we searched two mammalian genomes to identify potential epistatic interactions by looking for co-adapted genes marked by excess two-locus genetic differentiation between populations/lineages using publicly available SNP genotype data. The practical motivation for this effort is to reduce the number of pair-wise tests that need to be performed in genome-wide association studies aimed at detecting GxG interactions, by focusing on pairs predicted to be more likely to jointly affect variation in complex traits. Hence, this approach generates a list of candidates interactions that can be empirically tested. In both the mouse and human data we observed two-locus genetic differentiation in excess of what can be expected from chance alone based on simulations. In an attempt to validate our hypothesis that pairs of genes showing excess genetic divergence represent potential functional interactions we selected a small set of gene combinations postulated to be interacting based on our analyses and looked for a combined effect of the selected genes on variation in complex traits both mice and man. In both cases the individual effect of the genes were not significant. Instead we observed marginally significant interaction effects. These results show that genome wide searches for gene-gene interactions based on population genetic data are feasible and can generate interesting candidate gene pairs to be further tested for their contribution to phenotypic variation in complex traits. © 2008 Bochdanovits et al.

Published

2008

32. Testing replication of a 5-SNP set for general cognitive ability in six population samples

Author

Nicholas G. Martin, Margaret J. Wright, Michelle Luciano, Sarah E. Harris, Lawrence J. Whalley, Zoltán Bochdanovits, Eco J. C. de Geus, Danielle Posthuma, Grant W. Montgomery, Lee M. Butcher, Dorret I. Boomsma, Robert Plomin, Tinca J. C. Polderman, Penelope A. Lind, Ian J. Deary, Antony Payton, John M. Starr, Timothy C. Bates, Oliver S. P. Davis, Peter M. Visscher, Human genetics, Neuroscience Campus Amsterdam 2008, and Biological Psychology

Subjects

Netherlands Twin Register (NTR), Adult, Male, Adolescent, Population, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Correlation, 03 medical and health sciences, 0302 clinical medicine, Cognition, Meta-Analysis as Topic, Polymorphism (computer science), Genetics, Twins, Dizygotic, SNP, Humans, education, Child, Genetics (clinical), 030304 developmental biology, 0303 health sciences, education.field_of_study, Twins, Monozygotic, Twin study, Child, Preschool, Female, Twins Early Development Study, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

A 5-single nucleotide polymorphism (SNP) set has been associated with general cognitive ability in 5000 7-year-old children from the Twins Early Development Study (TEDS). Four of these SNPs were identified through a 10K microarray analysis and one was identified through a targeted analysis of brain-expressed genes. The present study tested this association with general cognitive ability in six population samples of varying size and age from Australia, the UK (Scotland and England) and the Netherlands. Results from the largest sample (N=1310) approached significance (P = 0.06) in the direction of the original finding, but results from the other samples (N = 205-758) were mixed. A meta-analysis of the results - allowing for effect size heterogeneity between samples - yielded a non-significant correlation (r = -0.01, P = 0.57), indicating that this SNP set was not associated with general cognitive ability in the populations studied.

Published

2008

33. P1–127: Distinguishing neurodegenerative disorders with tau pathology using MRNA expression microarrays

Author

Patrizia Rizzu, Peter Heutink, Zoltán Bochdanovits, John C. van Swieten, Wouter Kamphorst, Iraad F. Bronner, and Rivka Ravid

Subjects

Pathology, medicine.medical_specialty, Tau pathology, Epidemiology, Health Policy, Mrna expression, Biology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, medicine, Neurology (clinical), Geriatrics and Gerontology, DNA microarray

Published

2006

34. Antagonistic pleiotropy for life-history traits at the gene expression level

Author

Zoltán Bochdanovits and Gerdien de Jong

Subjects

Costa Rica, Male, Washington, Gene Expression, General Biochemistry, Genetics and Molecular Biology, Life history theory, Pleiotropy, Gene expression, Protein biosynthesis, Animals, Gene, General Environmental Science, Oligonucleotide Array Sequence Analysis, Genetics, Life Cycle Stages, General Immunology and Microbiology, biology, Mechanism (biology), General Medicine, biology.organism_classification, Adaptation, Physiological, Hedgehog signaling pathway, Drosophila melanogaster, Larva, Body Constitution, Female, General Agricultural and Biological Sciences, Energy Metabolism, Research Article

Abstract

Life–history trade–offs prevent different components of fitness from being maximized simultaneously. Although the existence of trade–offs has been clearly demonstrated, the ‘classical’ mechanism of adaptive resource allocation that should underlie them has recently received criticism. In this study, we explore the molecular mechanisms of life–history trade–offs by applying a quantitative genomic approach. Analysis of global gene expression in Drosophila melanogaster revealed 34 genes whose expression coincided with the genetic trade–off between larval survival and adult size. The joint expression of these candidate ‘trade–off’ genes explained 86.3% of the trade–off. Fourteen of these genes have known functions which suggest that the larval survival–adult size trade–off could be the result of resource allocation at the organismal level, but at the level of cellular metabolism the trade–off would reduce to a shift between energy metabolism versus protein biosynthesis, regulated by the RAS signalling pathway.

Published

2004

35. Experimental evolution in Drosophila melanogaster: interaction of temperature and food quality selection regimes

Author

Zoltán Bochdanovits and Gerdien de Jong

Subjects

Resource (biology), media_common.quotation_subject, Longevity, Biology, Resource Acquisition Is Initialization, Genetics, Animals, Selection, Genetic, Selection (genetic algorithm), Ecology, Evolution, Behavior and Systematics, media_common, Larva, Experimental evolution, Analysis of Variance, Ecology, Mechanism (biology), fungi, Temperature, Feeding Behavior, Biological Evolution, Drosophila melanogaster, Food, Body Constitution, Adaptation, General Agricultural and Biological Sciences

Abstract

In Drosophila, both the phenotypic and evolutionary effect of temperature on adult size involves alterations to larval resource processing and affects other life-history traits, that is, development time but most notably, larval survival. Therefore, thermal evolution of adult body size might not be independent of simultaneous adaptation of larval traits to resource availability. Using experimental evolution lines adapted to high and low temperatures at different levels of food, we show that selection pressures interact in shaping larval resource processing. Evolution on poor food invariably leads to lower resource acquisition suggesting a cost to feeding behavior. However, following low temperature selection, lower resource acquisition led to a higher adult body size, probably by more efficient allocation to growth. In contrast, following high temperature selection, low resource acquisition benefited larval survival, possibly by reducing feeding-associated costs. We show that evolved differences to larval resource processing provide a possible proximate mechanism to variation in a suite of correlated life-history traits during adaptation to different climates. The implication for natural populations is that in nature, thermal evolution drives populations to opposite ends of an adult size versus larval survival trade-off by altering resource processing, if resource availability is limited.

Published

2003

36. P3.032 Differences in gene expression patterns in the olfactory bulb of Parkinson patients and related disorders?

Author

Henk J. Groenewegen, Patrizia Rizzu, Zoltán Bochdanovits, J. M. Rozemuller, P. Voorn, Angela Ingrassia, W.D.J. van de Berg, Peter Heutink, and Anke A. Dijkstra

Subjects

Olfactory system, Neurology, Gene expression, Neurology (clinical), Geriatrics and Gerontology, Biology, Neuroscience, Olfactory bulb

Published

2009