Molecular Psychiatry: Sequence variations of ABCB1, SLC6A2, SLC6A3, SLC6A4, CREB1, CRHR1 and NTRK2: association with major depression and antidepressant response in Mexican

Tuesday, November 3, 2009

Sequence variations of ABCB1, SLC6A2, SLC6A3, SLC6A4, CREB1, CRHR1 and NTRK2: association with major depression and antidepressant response in Mexican

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Molecular Psychiatry advance online publication 20 October 2009; doi: 10.1038/mp.2009.92

C Dong¹, M-L Wong² and J Licinio²

Department of Psychiatry and Behavioral Sciences, Center for Pharmacogenomics, University of Miami Miller School of Medicine, Miami, FL, USA
John Curtin School of Medical Research, The Australian National University, Canberra, ACT, Australia

Correspondence: Professor J Licinio, John Curtin School of Medical Research, The Australian National University, GPO Box 334, Canberra, ACT 2601, Australia. E-mail: julio.licinio@anu.edu.au

Received 20 July 2009; Accepted 28 July 2009; Published online 20 October 2009.

Abstract

We studied seven genes that reflect events relevant to antidepressant action at four sequential levels: (1) entry into the brain, (2) binding to monoaminergic transporters, and (3) distal effects at the transcription level, resulting in (4) changes in neurotrophin and neuropeptide receptors. Those genes are ATP-binding cassette subfamily B member 1 (ABCB1), the noradrenaline, dopamine, and serotonin transporters (SLC6A2, SLC6A3 and SLC6A4), cyclic AMP-responsive element binding protein 1 (CREB1), corticotropin-releasing hormone receptor 1 (CRHR1) and neurotrophic tyrosine kinase type 2 receptor (NTRK2). Sequence variability for those genes was obtained in exonic and flanking regions. A total of 56 280 000 bp across were sequenced in 536 unrelated Mexican Americans from Los Angeles (264 controls and 272 major depressive disorder (MDD)). We detected in those individuals 419 single nucleotide polymorphisms (SNPs); the nucleotide diversity was 0.00054 plusminus 0.0001. Of those, a total of 204 novel SNPs were identified, corresponding to 49% of all previously reported SNPs in those genes: 72 were in untranslated regions, 19 were in coding sequences of which 7 were non-synonymous, 86 were intronic and 27 were in upstream/downstream regions. Several SNPs or haplotypes in ABCB1, SLC6A2, SLC6A3, SLC6A4, CREB1 and NTRK2 were associated with MDD, and in ABCB1, SLC6A2 and NTRK2 with antidepressant response. After controlling for age, gender and baseline 21-item Hamilton Depression Rating Scale (HAM-D21) score, as well as correcting for multiple testing, the relative reduction of HAM-D21 score remained significantly associated with two NTRK2-coding SNPs (rs2289657 and rs56142442) and the haplotype CAG at rs2289658 (splice site), rs2289657 and rs2289656. Further studies in larger independent samples will be needed to confirm these associations. Our data indicate that extensive assessment of sequence variability may contribute to increase understanding of disease susceptibility and drug response. Moreover, these results highlight the importance of direct re-sequencing of key candidate genes in ethnic minority groups in order to discover novel genetic variants that cannot be simply inferred from existing databases.

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My latest editorial - May 2009

Update on Molecular Psychiatry:
New publication guidelines and new ways to stay current

The field of molecular psychiatry has evolved considerably from when Molecular Psychiatry was launched in 1996. We present here brief and updated guidelines for publication as well as details on two innovative electronic resources – our blog and twitter.

We now receive over 700 manuscripts annually and can only publish a very small fraction of what we receive. In the light of the resulting high rejection rate, I am often asked what type of paper has the highest likelihood of acceptance. Here are some guidelines on the content and format that can lead to the highest likelihood of success.

On the important point of content, we seek work that is either conceptually novel or persuasively conclusive and that advances the field. Given the growth of approaches in psychiatric research, we are very open to the most diverse range of papers: from the epidemiological all the way to the most fundamental basic science, including in that broad range all aspects of translational and clinical research, pharmacology, genetics, genomics, proteomics, metabolomics, imaging, behavior, and animal-model research. I cannot think of an innovative, ground breaking or conclusive paper relevant to psychiatry that we would not be interested in. What is important is not so much the area, but either innovation and conceptual novelty or a definitive study that provides conclusive evidence.

Regarding format: because of the tremendous pressure on our space, brevity is encouraged. Most scientific work can benefit from a careful format and style revision aimed at achieving maximum clarity and brevity. Frankly, while your own story may be captivating to you, neither reviewers nor readers have the time or the disposition to go through pages and pages of details or speculation. Please build your paper around data and provide a succinct description of what led you to collect those data, including the guiding hypotheses and methods used, and then provide a brief discussion of your results in the context of where that particular area of research is now and where it is going. We will not publish your article if your results cannot speak for themselves and you need thousands of words of introduction and discussion to highlight them.

One of our goals has been to foster dialogue in the field. Originally, that occurred in our Letters to the Editor and News & Commentary sections. However, the competition for our space makes the fostering of such dialogue increasingly difficult, as it is hard to justify rejecting a highly meritorious paper for lack of space as we dedicate space to interesting, but not critical, correspondence. Furthermore, there is now an increasing discrepancy between the immediacy of electronic publishing and the time constraints of print. In order to facilitate a dialogue in the field and to rapidly alert authors to emerging articles, I am personally creating two new resources for the field that will be mostly related to Molecular Psychiatry, but will occasionally include updates, news, and comments on other material that is of relevance to our field. Those resources are a new Molecular Psychiatry blog and a twitter.

The Molecular Psychiatry blog can be found at http://molecularpsychiatry.blogspot.com. In this blog we will give authors the option to provide summaries of their papers with links to the journal site containing the full article. Those summaries would appear in the blog in conjunction with Advance Online Publication. A dialogue around the paper and its subject matter can then rapidly develop in real-time with comments, questions and answers from the scientific community at large. Authors are not required to respond to comments, but may do so if they feel appropriate. As a safety measure, I will moderate this blog; therefore, material will only be posted with my approval. This will protect authors from inappropriate comments or nuisance. Having grown up in a military dictatorship that enforced official censorship of the press, I have a heartfelt commitment to freedom of speech and will only screen out truly inappropriate blog submissions. Authors and the public can e-mail me if they think that my screening is inappropriate. It is hoped that the blog will foster a lively real-time dialogue that will energize authors and readers.

Our second outreach innovation will be through twitter. For those interested in twittering on Molecular Psychiatry, just go into your twitter account and search for “Julio Licinio.” Subscribe to my open twitter and as any exciting development emerges in Molecular Psychiatry or in other publications, I will twitter about those. For my older colleagues who do not know what twitter is, please get a tutorial from your children, grandchildren, or young relatives, students, or anyone under 30. You can also go to http://www.twitter.com. Briefly, by subscribing to twitter you can tell others or hear from others what is happening now. I am using my twitter to rapidly disseminate exciting emerging data with relevant weblinks. The beauty of twitter is that each message can have a maximum of 140 characters. Those brief notifications are sufficient to keep you in touch with the latest findings, without the unnecessary distraction that would be caused by lengthy texts. I will mostly twitter take-home summaries of interesting papers as soon as they come out in Molecular Psychiatry online (ahead of print). Occasional twitters of groundbreaking work in the field, published elsewhere, will also be sent out – in moderation – as alerts of critical new data, without overwhelming your mailboxes.

Julio Licinio
Editor

Molecular Psychiatry

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Tuesday, November 3, 2009

Sequence variations of ABCB1, SLC6A2, SLC6A3, SLC6A4, CREB1, CRHR1 and NTRK2: association with major depression and antidepressant response in Mexican

Original Article

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Post a Comment

Twitter on Molecular Psychiatry

Our current issue

About Me

Molecular Psychiatry Website

Molecular Psychiatry TOP TEN

NEW FEATURE FOR AUTHORS

NatureNews

Science jobs

Some interesting links

My latest editorial - May 2009

Blog Archive

Molecular Psychiatry

WELCOME

Tuesday, November 3, 2009

Sequence variations of ABCB1, SLC6A2, SLC6A3, SLC6A4, CREB1, CRHR1 and NTRK2: association with major depression and antidepressant response in Mexican

Original Article

No comments:

Post a Comment

Twitter on Molecular Psychiatry

Our current issue

About Me

Molecular Psychiatry Website

Molecular Psychiatry TOP TEN

NEW FEATURE FOR AUTHORS

Subscribe To

NatureNews

Science jobs

Some interesting links

My latest editorial - May 2009

Blog Archive