Literature DB >> 11992563

Genome survey for susceptibility loci for recurrent, early-onset major depression: results at 10cM resolution.

George S Zubenko1, Hugh B Hughes, J Scott Stiffler, Wendy N Zubenko, Barry B Kaplan.   

Abstract

Recurrent (two or more episodes), early-onset (first episode at < or = 25 years) major depressive disorder (RE-MDD) is a strongly familial condition (lambda(first-degree relatives) = 8) whose malignant effects have a significant negative impact on the health and longevity of patients and their family members. The goal of this study was to identify candidate susceptibility loci that influence the development of RE-MDD. We completed a systematic survey of the human genome, conducted at an average resolution of 10 cM, for the identification of simple sequence tandem repeat polymorphisms (SSTRPs) that target susceptibility genes for RE-MDD by virtue of linkage disequilibrium. The efficiency of our association study was enhanced by genotyping pools of DNA from 100 adults with RE-MDD and 100 adult controls who had no personal or family history of mental disorders. Both groups included equal numbers of Caucasian men and women and were matched as closely as possible for age and ethnicity. Allelic associations with RE-MDD were observed for 19 of the 387 SSTRPs in the CHLC Human Screening Set/Weber Version 9. Sixteen of the 19 candidate susceptibility loci revealed significant allelic associations with RE-MDD in men (n = 7) or women (n = 9), but not in both sexes. Evidence for both risk and protective alleles was detected. Two of the candidate susceptibility loci reside within several Mb of loci previously reported-megabases to be linked to "comorbid alcoholism and depression" in families of individuals with alcoholism and to a broadly defined affected phenotype that included recurrent major depression in the families of patients with bipolar disorder. Although it has been suggested that the genes that influence risk for MDD in the two sexes may not be entirely the same, the results of our study suggest that sex specificity of susceptibility loci for RE-MDD may be the rule rather than the exception. The observed preponderance of sex-specific susceptibility loci for RE-MDD suggests that there may be important differences in the molecular pathophysiology of RE-MDD in men and women. Alternatively, our findings may reflect the existence of sex-specific differences in the molecular mechanisms that determine resilience to endogenous or environmental depressogenic stimuli. Copyright 2002 Wiley-Liss, Inc.

Entities:  

Mesh:

Year:  2002        PMID: 11992563     DOI: 10.1002/ajmg.10381

Source DB:  PubMed          Journal:  Am J Med Genet        ISSN: 0148-7299


  16 in total

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Journal:  Mol Diagn Ther       Date:  2014-10       Impact factor: 4.074

2.  Preferences regarding targeted education and risk assessment in people with a family history of major depressive disorder.

Authors:  Veronica Quinn; Bettina Meiser; Alex Wilde; Zoe Cousins; Kristine Barlow-Stewart; Philip B Mitchell; Peter R Schofield
Journal:  J Genet Couns       Date:  2014-01-10       Impact factor: 2.537

3.  Replacement of homologous mouse DNA sequence with pathogenic 6-base human CREB1 promoter sequence creates murine model of major depressive disorder.

Authors:  George S Zubenko; Hugh B Hughes
Journal:  Am J Med Genet B Neuropsychiatr Genet       Date:  2011-05-19       Impact factor: 3.568

4.  Genome-wide linkage scan of antisocial behavior, depression, and impulsive substance use in the UCSF family alcoholism study.

Authors:  Ian R Gizer; Cindy L Ehlers; Cassandra Vieten; Heidi S Feiler; David A Gilder; Kirk C Wilhelmsen
Journal:  Psychiatr Genet       Date:  2012-10       Impact factor: 2.458

5.  Genetic linkage of region containing the CREB1 gene to depressive disorders in families with recurrent, early-onset, major depression: a re-analysis and confirmation of sex-specific effect.

Authors:  Brion S Maher; Hugh B Hughes; Wendy N Zubenko; George S Zubenko
Journal:  Am J Med Genet B Neuropsychiatr Genet       Date:  2010-01-05       Impact factor: 3.568

6.  A novel analytical framework for dissecting the genetic architecture of behavioral symptoms in neuropsychiatric disorders.

Authors:  Anthony J Deo; Ramiro Costa; Lynn E DeLisi; Rob DeSalle; Fatemeh Haghighi
Journal:  PLoS One       Date:  2010-03-16       Impact factor: 3.240

7.  Exploring culture-specific differences in beliefs about causes, kinship and the heritability of major depressive disorder: the views of Anglo-Celtic and Chinese-Australians.

Authors:  Mimi Xu; Lilian Zou; Alex Wilde; Bettina Meiser; Kristine Barlow-Stewart; Bibiana Chan; Philip B Mitchell; Mariana S Sousa; Peter R Schofield
Journal:  J Genet Couns       Date:  2013-05-17       Impact factor: 2.537

8.  Predisposition locus for major depression at chromosome 12q22-12q23.2.

Authors:  Victor Abkevich; Nicola J Camp; Charles H Hensel; Chris D Neff; Deanna L Russell; Dana C Hughes; Agnes M Plenk; Michael R Lowry; R Lynn Richards; Catherine Carter; Georges C Frech; Steven Stone; Kerry Rowe; Chi Ai Chau; Kathleen Cortado; Angelene Hunt; Karanina Luce; Gayanne O'Neil; Jeff Poarch; Jennifer Potter; Gregg H Poulsen; Heidi Saxton; Michelle Bernat-Sestak; Victor Thompson; Alexander Gutin; Mark H Skolnick; Donna Shattuck; Lisa Cannon-Albright
Journal:  Am J Hum Genet       Date:  2003-11-05       Impact factor: 11.025

9.  Effects of the G(-656)A variant on CREB1 promoter activity in a neuronal cell line: interactions with gonadal steroids and stress.

Authors:  G S Zubenko; H B Hughes
Journal:  Mol Psychiatry       Date:  2008-03-04       Impact factor: 15.992

10.  Genetic epidemiology of self-reported lifetime DSM-IV major depressive disorder in a population-based twin sample of female adolescents.

Authors:  Anne L Glowinski; Pamela A F Madden; Kathleen K Bucholz; Michael T Lynskey; Andrew C Heath
Journal:  J Child Psychol Psychiatry       Date:  2003-10       Impact factor: 8.982

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