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Featured researches published by Df Levinson.


Schizophrenia Research | 1998

A transmission disequilibrium and linkage analysis of D22S278 marker alleles in 574 families: further support for a susceptibility locus for schizophrenia at 22q12

Homero Vallada; David Curtis; Pak Sham; Hiroshi Kunugi; Jinghua Zhao; Robin M. Murray; P. McGuffin; Shinichiro Nanko; Michael John Owen; Michael Gill; D. A. Collier; David E. Housman; Haig H. Kazazian; Gerald Nestadt; Ann E. Pulver; Richard E. Straub; Charles J. MacLean; Dermot Walsh; Kenneth S. Kendler; Lynn E. DeLisi; M Polymeropoulos; Hilary Coon; William Byerley; R. Lofthouse; Elliot S. Gershon; Lynn R. Goldin; Robert Freedman; Claudine Laurent; S BodeauPean; Thierry d'Amato

Patients with schizophrenia rarely develop rheumatoid arthritis, an autoimmune disease that exhibits genetic association with the HLA DRB1*04 gene. We previously investigated the hypothesis that schizophrenia is negatively associated with DRB1*04, and found that only half the expected number of schizophrenic patients had this gene when compared with controls. We now report the results of DRB1*04 genotyping in pedigrees multiply affected with schizophrenia. Polymerase chain reaction amplification and sequence-specific oligonucleotide probes were used to determine the DRB1 genotypes of the 187 members of 23 pedigrees multiply affected with RDC schizophrenia. DQA1, DQB1 and DPB1 genotypes were similarly determined. We analysed data using the extended transmission/disequilibrium test and found a trend for the preferential non-transmission of DRB1*04 alleles from heterozygous parents to their schizophrenic offspring (16 of 23 alleles not transmitted, chi 2 = 3.5, p = 0.06). We found no evidence for a gene of major effect using GENEHUNTER for parametric and non-parametric linkage analysis. The results from this small sample need to be interpreted with caution, but they are in keeping with previous reports and suggest that HLA DRB1*04 alleles may be associated with a reduced risk of schizophrenia.Previously, a combined analysis by the Chromosome 22 Collaborative Linkage Group (1996; Am. J. Med Genet. 67, 40-45) used an affected sib-pair analysis of a single marker (D22S278) in 574 families multiply affected by schizophrenia and found some evidence for linkage (chi 2 = 9.35, 1 df, p = 0.001), suggesting the presence of a disease locus nearby on chromosome 22q12. In order to further investigate the importance of this result, we have performed the transmission disequilibrium test (TDT) and additional parametric and non-parametric linkage analysis of the same data. The most positive result obtained was an admixture lod score of 0.9 under the assumption of locus heterogeneity and dominant transmission. The result of the TDT analysis was significant at p = 0.015 (allele-wise; chi 2 = 22, 10 df) and p = 0.00016 (genotype-wise; chi 2 = 66.2, 30 df, empirical p value = 0.0009). Overall, these results further strengthen the notion that there is a susceptibility locus for schizophrenia close to D22S278.


Annals of Human Genetics | 2008

Extended meta-analysis of genome-wide linkage studies in schizophrenia

Cathryn M. Lewis; Mandy Y.M. Ng; Df Levinson

Bertram Müller‐Myhsok


American Journal of Medical Genetics | 2002

Meta-analysis of genome scans for schizophrenia

Cathryn M. Lewis; Lesley H. Wise; Df Levinson


Genetic Epidemiology | 2005

Testing for heterogeneity of linkage in meta-analysis studies.

Cathryn M. Lewis; Df Levinson


American Journal of Medical Genetics | 2004

Polymorphisms in trace amine receptor 4 (TRAR4) are associated with susceptibility for schizophrenia on chromosome 6q23.2

Jubao Duan; Maria Martinez; Alan R. Sanders; Cuiping Hou; Naruya Saitou; Takashi Kitano; Bryan J. Mowry; Raymond R. Crowe; J. M. Silverman; Df Levinson; P. V. Gejman


American Journal of Medical Genetics | 1998

Mutational analysis of the 5-HT1B and 5-HT1E serotonin receptor genes in three datasets with schizophrenia

Jennifer Taylor; Qiuhe Cao; Anibal Cravchik; Judith Badner; Bryan J. Mowry; Df Levinson; Raymond R. Crowe; J. M. Silverman; Lynn R. Goldin; Elliot S. Gershon; Pablo V. Gejman


Biological Psychiatry | 2017

Does Childhood Trauma Moderate Polygenic Risk for Depression?: A Meta-analysis of 5765 Subjects From the Psychiatric Genomics Consortium

Wouter J. Peyrot; Sandra Van der Auwera; Yuri Milaneschi; Conor V. Dolan; Pamela A. F. Madden; Patrick F. Sullivan; Jana Strohmaier; Stephan Ripke; Marcella Rietschel; Michel G. Nivard; Niamh Mullins; G W Montgomery; Anjali K. Henders; Andrew C. Heat; Helen L. Fisher; Erin C. Dunn; Enda M. Byrne; Tracy A. Air; Bernhard T. Baune; Gerome Breen; Df Levinson; Cathryn M. Lewis; Nicholas G. Martin; Elliot N. Nelson; Dorret I. Boomsma; Hans Jörgen Grabe; Naomi R. Wray; Brenda W.J.H. Penninx


American Journal of Human Genetics | 2003

Linkage disequilibrium analysis of single nucleotide polymorphisms of the glutamate receptor 6 gene and schizophrenia

Maria Martinez; Alan R. Sanders; L Martinolich; Eb Carpenter; Jubao Duan; Bryan J. Mowry; Df Levinson; Raymond R. Crowe; J. M. Silverman; Pablo V. Gejman


American Journal of Human Genetics | 2002

Linkage disequillbrium analysis of 6ql3-q26 schizophrenia candidate genes.

Alan R. Sanders; Maria Martinez; L Martinolich; Eb Carpenter; Jubao Duan; Bryan J. Mowry; Df Levinson; Raymond R. Crowe; J. M. Silverman; Pablo V. Gejman


Molecular Psychiatry | 1999

Genome scan of schizophrenia: Results of genotyping of positive regions.

Df Levinson; Bryan J. Mowry; Kelly R. Ewen; Derek J. Nancarrow; Nicholas K. Hayward; Raymond R. Crowe; Nancy C. Andreasen; Donald W. Black; J. M. Silverman; Jean Endicott; Lawrence Sharpe; Richard C. Mohs; Larry J. Siever; Marilyn K. Walters; David P. Lennon; Deborah A. Nertney; Simon J. Foote

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Bryan J. Mowry

University of Queensland

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J. M. Silverman

University of Pennsylvania

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Donald W. Black

Roy J. and Lucille A. Carver College of Medicine

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P. V. Gejman

University of Illinois at Chicago

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