Your search keyword '"David P. Lennon"' showing total 8 results

1. No support for linkage to the bipolar regions on chromosomes 4p, 18p, or 18q in 43 schizophrenia pedigrees

Author

Donna M. Brown, Nicholas K. Hayward, Marilyn K. Walters, Larry J. Siever, Deborah A. Nertney, Nancy C. Andreasen, Richard C. Mohs, Bryan J. Mowry, Helen L. Jones, Leonid Kruglyak, Andrew Kirby, David P. Lennon, Melanie M. Mahtani, Derek J. Nancarrow, Jennifer M. Taylor, Douglas F. Levinson, Donald W. Black, Jean Endicott, Raymond R. Crowe, Jeremy M. Silverman, and Lawrence Sharpe

Subjects

Linkage (software), Bipolar Disorder, Genetic Linkage, Schizophrenia (object-oriented programming), Context (language use), Pedigree chart, Susceptibility gene, Biology, Population stratification, Pedigree, Evolutionary biology, mental disorders, Individual data, Schizophrenia, Humans, Chromosomes, Human, Pair 4, Chromosomes, Human, Pair 18, Gene, Genetics (clinical)

Abstract

These data provide no support for the hypothesis that a schizophrenia susceptibility gene of major to moderate effect within our data set maps to one of these bipolar susceptibility regions on 4p, 18p, and 18q. When our results are considered in the context of those from other researchers, two explanations arise: either the initially positive scores within these regions are the result of type one linkage errors (false positive scores); or a gene(s) of small effect for BPAD, schizophrenia, or both, maps to one or more of these regions. Given issues of power and population stratification in individual data sets, identifying such genes of small effect remains a challenge for the field.© 2000 Wiley-Liss, Inc.

Published

2000

2. Second stage of a genome scan of schizophrenia: Study of five positive regions in an expanded sample

Author

Jeremy M. Silverman, Douglas F. Levinson, Lawrence Sharpe, Catherine E. Thornley, Nicholas K. Hayward, Jean Endicott, Kelly R. Ewen, Raymond R. Crowe, Deborah A. Nertney, Matthew S. O'Brien, Madeline M. Gladis, Bryan J. Mowry, Helen L. Jones, Simon J. Foote, Marilyn K. Walters, David P. Lennon, and Derek J. Nancarrow

Subjects

Linkage (software), Genetics, Schizophrenia, Genetic linkage, medicine, Chromosome, Genome Scan, Pedigree chart, Biology, medicine.disease, Genome, Genetics (clinical), Genetic determinism

Abstract

In a previous genome scan of 43 schizophrenia pedigrees, nonparametric linkage (NPL) scores with empirically derived pointwise P-values less than 0.01 were observed in two regions (chromosomes 2q12-13 and 10q23) and less than 0.05 in three regions (4q22-23, 9q22, and 11q21). Markers with a mean spacing of about 5 cM were typed in these regions in an expanded sample of 71 pedigrees, and NPL analyses carried out. No region produced significant genomewide evidence for linkage. On chromosome 10q, the empirical P-value remained at less than 0.01 for the entire sample (D10S168), evidence in the original 43 pedigrees was slightly increased, and a broad peak of positive results was observed. P-values less than 0.05 were observed on chromosomes 2q (D2S436) and 4q (D4S2623), but not on chromosomes 9q or 11q. It is concluded that this sample is most supportive of linkage on chromosome 10q, with less consistent support on chromosomes 2q and 4q. Am. J. Med. Genet. (Neuropsychiatr. Genet.) 96:864-869, 2000. © 2000 Wiley-Liss, Inc.

Published

2000

3. Follow-up study on a susceptibility locus for schizophrenia on chromosome 6q

Author

Derek J. Nancarrow, Bryan J. Mowry, Pablo V. Gejman, Lynn R. Goldin, Donna M. Brown, Elliot S. Gershon, Nancy C. Andreasen, David P. Lennon, Donald W. Black, Raymond R. Crowe, Quihe Cao, Jennifer M. Taylor, Maria Martinez, Douglas F. Levinson, Jing Zhang, Deborah A. Nertney, Jeremy M. Silverman, Andrew Kirby, and Alan R. Sanders

Subjects

Linkage (software), Genetics, Candidate gene, Genetic linkage, Sample size determination, Chromosome, Microsatellite, Pedigree chart, Biology, Genetics (clinical), Genetic determinism

Abstract

Evidence for suggestive linkage to schizophrenia with chromosome 6q markers was previously reported from a two-stage approach. Using nonparametric affected sib pairs (ASP) methods, nominal p-values of 0.00018 and 0.00095 were obtained in the screening (81 ASPs; 63 independent) and the replication (109 ASPs; 87 independent) data sets, respectively. Here, we report a follow-up study of this 50cM 6q region using 12 microsatellite markers to test for linkage to schizophrenia. We increased the replication sample size by adding an independent sample of 43 multiplex pedigrees (66 ASPs; 54 independent). Pairwise and multipoint nonparametric linkage analyses conducted in this third data set showed evidence consistent with excess sharing in this 6q region, though the statistical level is weaker (p=0.013). When combining both replication data sets (total of 141 independent ASPs), an overall nominal p-value=0.000014 (LOD=3.82) was obtained. The sibling recurrence risk (λs) attributed to this putative 6q susceptibility locus is estimated to be 1.92. The linkage region could not be narrowed down since LOD score values greater than three were observed within a 13cM region. The length of this region was only slightly reduced (12cM) when using the total sample of independent ASPs (204) obtained from all three data sets. This suggests that very large sample sizes may be needed to narrow down this region by ASP linkage methods. Study of the etiological candidate genes in this region is ongoing.

Published

1999

4. Puerperal Psychosis: Associated Clinical Features in a Psychiatric Hospital Mother-Baby Unit

Author

Bryan J. Mowry and David P. Lennon

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Psychiatric Department, Hospital, Personality Assessment, Diagnostic system, Foster Home Care, Unit (housing), 03 medical and health sciences, Child Rearing, Patient Admission, 0302 clinical medicine, Hostility, Humans, Medicine, Psychiatric hospital, 030212 general & internal medicine, Psychiatry, Retrospective Studies, Psychiatric Status Rating Scales, Puerperal psychosis, business.industry, Infant, Newborn, Infant, Puerperal Disorders, General Medicine, Middle Aged, medicine.disease, Mother-Child Relations, 030227 psychiatry, Psychiatry and Mental health, Psychotic Disorders, Female, Postpartum psychosis, business, Separate legal entity

Abstract

Objective: Current psychiatric diagnostic systems do not regard puerperal psychosis as a separate entity. However, there is continuing debate about the validity and clinical utility of this concept. This paper aims to investigate the prognostic importance of a number of clinical features in a sample of patients with puerperal psychosis. Method: A retrospective case note study was conducted on 42 consecutive admissions to a mother-baby unit in a psychiatric hospital. Data were collected on a range of variables, and diagnoses made according to DSM-III-R and RDC criteria for puerperal psychosis. Results: Maternal hostility toward the baby was the only studied variable to increase the likelihood of the baby being cared for by someone other than the mother, indicating the mother's inability to safely care for the baby. Conclusions: These findings tentatively suggest that it is maternal hostility toward the baby, not puerperal psychosis per se that is associated with foster care.

Published

1998

5. A linkage study of schizophrenia to markers within Xp11 near the MAOB gene

Author

Margot Albus, Angela B. Smith, S. H. Laval, Marcella Devoto, David P. Lennon, David A. Collier, Giordano Invernizzi, Lynn E. DeLisi, Douglas F. Levinson, Paula Peterson, Bernard Lerer, Robin M. Murray, Raymond R. Crowe, Margherita Comazzi, Wolfgang Maier, John Powell, Richard C. Mohs, Bryan J. Mowry, Nicholas K. Hayward, Timothy J. Crow, Jeremy M. Silverman, J. Loftus, Nancy C. Andreasen, Derek J. Nancarrow, Janine Dann, Dieter B. Wildenauer, Antonio Vita, Gail Shields, and Marilyn K. Walters

Subjects

Genetic Markers, Psychosis, X Chromosome, Genetic Linkage, Genes, Recessive, Locus (genetics), Schizoaffective disorder, Cohort Studies, Gene mapping, medicine, Humans, Monoamine Oxidase, Gene, Sex Chromosome Aberrations, Biological Psychiatry, X chromosome, Genes, Dominant, Genetics, Models, Genetic, Chromosome Mapping, medicine.disease, Psychiatry and Mental health, Schizophrenia, Schizophrenic Psychology, Monoamine oxidase B, Lod Score, Psychology, Cohort study

Abstract

A sex chromosome locus for psychosis has been considered on the basis of some sex differences in genetic risk and expression of illness, and an association with X-chromosome anomalies. Previous molecular genetic studies produced weak evidence for linkage of schizophrenia to the proximal short arm of the X-chromosome, while some other regions were not ruled out. Here we report an attempt to expand the Xp findings in: (i) a multicenter collaboration focusing on 92 families with a maternal pattern of inheritance (Study I), and (ii) an independent sample of 34 families unselected for parental mode of transmission (Study II). In the multicenter study, a parametric analysis resulted in positive lod scores (highest of 1.97 for dominant and 1.19 for recessive inheritance at a theta of 0.20) for locus DXS7, with scores below 0.50 for other markers in this region (MAOB, DXS228, and ARAF1). Significant allele sharing among affected sibling pairs was present at DXS7. In the second study, positive lod scores were observed at MAOB (highest of 2.16 at a theta of 0.05 for dominant and 1.64 at a theta of 0.00 for recessive models) and ALAS2 (the highest of 1.36 at a theta of 0.05 for a recessive model), with significant allele sharing (P = 0.003 and 0.01, respectively) at these two loci. These five markers are mapped within a small region of Xp11. Thus, although substantial regions of the X-chromosome have been investigated without evidence for linkage being found, a locus predisposing to schizophrenia in the proximal short arm of the X-chromosome is not excluded.

Published

1997

6. Additional support for schizophrenia linkage on chromosomes 6 and 8: A multicenter study

Author

Dieter B. Wildenauer, Sibylle G. Schwab, Margot Albus, Joachim Hallmayer, Bernard Lerer, Wolfgang Maier, Douglas Blackwood, Walter Muir, David St Clair, Stewart Morris, Hans W. Moises, Liu Yang, Helgi Kristbjarnarson, Tomas Helgason, Claudia Wiese, David A. Collier, Peter Holmans, Jo Daniels, Mark Rees, Philip Asherson, Queta Roberts, Alastair Cardno, Maria J. Arranz, Homero Vallada, David Ball, Hiroshi Kunugi, Robin M. Murray, John F. Powell, Sin Nanko, Pak Sham, Mike Gill, Peter McGuffin, Michael J. Owen, Ann E. Pulver, Stylianos E. Antonarakis, Robert Babb, Jean-Louis Blouin, Nicola DeMarchi, Beth Dombroski, David Housman, Maria Karayiorgou, Jurg Ott, Laura Kasch, Haig Kazazian, Virginia K. Lasseter, Erika Loetscher, Hermann Luebbert, Gerald Nestadt, Carl Ton, Paula S. Wolyniec, Claudine Laurent, Michel de Chaldee, Florence Thibaut, Maurice Jay, Daniele Samolyk, Michel Petit, Dominique Campion, Jacques Mallet, Richard E. Straub, Charles J. MacLean, Stephen M. Easter, F. Anthony O'Neill, Dermot Walsh, Kenneth S. Kendler, Pablo V. Gejman, Qiuhe Cao, Elliot Gershon, Judith Badner, Ethiopia Beshah, Jing Zhang, Brien P. Riley, Swarnageetha Rajagopalan, Mpala Mogudi-Carter, Trefor Jenkins, Robert Williamson, Lynn E. DeLisi, Chad Garner, Mary Kelly, Carrie LeDuc, Lon Cardon, Jay Lichter, Tim Harris, Josephine Loftus, Gail Shields, Margarite Comasi, Antonio Vita, Angela Smith, Jay Dann, Geoff Joslyn, Hugh Gurling, Gursharan Kalsi, Jon Brynjolfsson, David Curtis, Thordur Sigmundsson, Robert Butler, Tim Read, Patrice Murphy, Andrew Chih-Hui Chen, Hannes Petursson, Bill Byerley, Mark Hoff, John Holik, Hilary Coon, Douglas F. Levinson, Derek J. Nancarrow, Raymond R. Crowe, Nancy Andreasen, Jeremy M. Silverman, Richard C. Mohs, Larry J. Siever, Jean Endicott, Lawrence Sharpe, Marilyn K. Walters, David P. Lennon, Nicholas K. Hayward, Lodewijk A. Sandkuijl, Bryan J. Mowry, Harald N. Aschauer, Kurt Meszaros, Elisabeth Lenzinger, Karoline Fuchs, Angela M. Heiden, Leonid Kruglyak, Mark J. Daly, and Tara C. Matise

Subjects

Genetics, Chromosome, Locus (genetics), Pedigree chart, Biology, Genetic linkage, Collaboration, Genotype levinson, Chromosome 3, Genetic marker, Polymorphism, Schizophrenia, Genotype, Microsatellite, Genetics (clinical)

Abstract

In response to reported schizophrenia linkage findings on chromosomes 3, 6 and 8, fourteen research groups genotyped 14 microsatellite markers in an unbiased, collaborative (New) sample of 403-567 informative pedigrees per marker, and in the Original sample which produced each finding (the Johns Hopkins University sample of 46-52 informative pedigrees for chromosomes 3 and 8, and the Medical College of Virginia sample of 156-191 informative pedigrees for chromosome 6). Primary planned analyses (New sample) were two-point heterogeneity lod score (lod2) tests (dominant and recessive affected-only models), and multipoint affected sibling pair (ASP) analysis, with a narrow diagnostic model (DSM-IIIR schizophrenia and schizoaffective disorders). Regions with positive results were also analyzed in the Original and Combined samples. There was no evidence for linkage on chromosome 3. For chromosome 6, ASP maximum lod scores (MLS) were 2.19 (New sample, nominal p = 0.001) and 2.68 (Combined sample, p = .0004). For chromosome 8, maximum lod2 scores (tests of linkage with heterogeneity) were 2.22 (New sample, p = .0014) and 3.06 (Combined sample, p = .00018). Results are interpreted as inconclusive but suggestive of linkage in the latter two regions. We discuss possible reasons for failing to achieve a conclusive result in this large sample. Design issues and limitations of this type of collaborative study are discussed, and it is concluded that multicenter follow-up linkage studies of complex disorders can help to direct research efforts toward promising regions.

Published

1996

7. Diagnosis of schizophrenia in a matched sample of Australian aborigines

Author

C N De Felice, Bryan J. Mowry, and David P. Lennon

Subjects

Adult, Cross-Cultural Comparison, Male, Psychosis, medicine.medical_specialty, Native Hawaiian or Other Pacific Islander, Psychometrics, Cross-sectional study, Schizophrenic Psychology, medicine, Psychiatric hospital, Humans, Psychiatry, Retrospective Studies, Psychiatric Status Rating Scales, Medical record, Incidence, Australia, Middle Aged, medicine.disease, Patient Discharge, Psychiatry and Mental health, Cross-Sectional Studies, Schizophrenia, Female, Psychology, Diagnosis of schizophrenia

Abstract

Cross-cultural phenomenology is one method of studying mental disorders such as schizophrenia. There are few data of this nature available on Australian aborigines. Using a retrospective medical record review of 39 matched pairs of aboriginal and nonaboriginal patients discharged as schizophrenic from a psychiatric hospital, this study investigated whether any phenomenological differences, using DSM-III-R criteria, existed between the two groups. Of all criteria, bizarre delusions, social deterioration, illness duration and organic exclusion were statistically significant, with fewer aboriginal subjects having documentation for each of these variables. Possible explanations for these findings, including intergroup phenomenological differences and assessment variation, are discussed.

Published

1994

8. A genome scan of schizophrenia

Author

Donna M. Brown, Jeremy M. Silverman, Mark J. Daly, Lawrence Sharpe, Marilyn K. Walters, Andrew Kirby, Derek J. Nancarrow, Raymond R. Crowe, Nicholas K. Hayward, Melanie M. Mahtani, Nancy C. Andreasen, Jean Endicott, Douglas F. Levinson, Richard C. Mohs, Bryan J. Mowry, Leonid Kruglyak, and David P. Lennon

Subjects

Psychiatry and Mental health, Schizophrenia (object-oriented programming), Genetics, Genome Scan, Computational biology, Biology, Biological Psychiatry, Genetics (clinical)

Published

1996