The American Journal of Psychiatry
Journal Home Search Current Issue Past Issues Subscribe All APPI Journals Help Contact Us
 
Am J Psychiatry Published March 17, 2008
doi: 10.1176/appi.ajp.2008.07060883
© 2008 American Psychiatric Association
Quicksearch
Advanced Search
Or Search All APPI Journals
This Article
* Full Text (PDF)
* Alert me when this article is cited
* Alert me if a correction is posted
Services
* Email this article to a Colleague
* Similar articles in this journal
* Similar articles in PubMed
* Alert me to new issues of the journal
* Add to My Articles & Searches
* Download to citation manager
* reprints & permissions
Google Scholar
* Articles by Rietschel, M.
* Articles by Schulze, T. G.
PubMed
* PubMed Citation
* Articles by Rietschel, M.
* Articles by Schulze, T. G.

G72 and Its Association With Major Depression and Neuroticism in Large Population-Based Groups From Germany

Marcella Rietschel, M.D., Lars Beckmann, Ph.D., Jana Strohmaier, M.Psych., Alexander Georgi, M.Psych., Anna Karpushova, Ph.D., Frederike Schirmbeck, M.Psych., Katja V. Boesshenz, M.A., Christine Schmäl, M.D., Christin Bürger, M.Psych., Rami Abou Jamra, M.D., Johannes Schumacher, M.D., Susanne Höfels, M.Psych., Robert Kumsta, Ph.D., Sonja Entringer, Ph.D., Axel Krug, M.Psych., Valentin Markov, M.Psych., Wolfgang Maier, M.D., Peter Propping, M.D., Stefan Wüst, Ph.D., Tilo Kircher, M.D., Markus M. Nöthen, M.D., Sven Cichon, Ph.D., and Thomas G. Schulze, M.D.

Objective: G72 is among the most frequently replicated vulnerability genes for schizophrenia and bipolar disorder. The authors previously found identical haplotypes of markers M23 and M24 to be associated with schizophrenia, bipolar disorder, and panic disorder. Given both the well-recognized familial clustering across these disorders and recent linkage findings implicating the region harboring G72 in the etiology of major depression and panic disorder, we can hypothesize that G72 should also be involved in the etiology of major depression. Neuroticism, measuring trait anxiety, may be the endophenotypic link underlying genetic associations with G72 across diagnostic boundaries. The authors tested whether the previously observed risk haplotypes are also associated with major depression and neuroticism. Method: The authors performed a standard haplotype analysis in a group of 500 major depression patients and 1,030 population-based comparison subjects. The authors also performed an exploratory analysis on 10 additional G72 markers using a novel haplotype-sharing approach. They performed a quantitative trait haplotype analysis in an independent group of 907 individuals phenotyped for neuroticism. Results: The previously identified M23-M24 risk haplotype was significantly associated with major depression and high levels of neuroticism. The haplotype-sharing analysis also implicated the same region, whereas more proximal markers showed no association with major depression. Conclusions: This is the first study to the authors' knowledge to implicate the G72 locus in the etiology of major depression and neuroticism. The results strengthen the notion of a genetic overlap between diagnoses, commonly conceptualized as distinct entities. Neuroticism may constitute the common underlying endophenotypic link.




Get information about faster international access.

Privacy Policy

Copyright © 2008 American Psychiatric Association. All rights reserved.

Home | Search | Current Issue | Past Issues | Subscribe | All APPI Journals | Help | Contact Us

American Psychiatric Publishing, Inc. American Psychiatric Association
1000 Wilson Boulevard, Suite 1825, Arlington, VA 22209-3901 * 800-368-5777 * appi at psych.org