Association of unipolar major depressive disorder with genes of the serotonergic and dopaminergic pathways

Frisch, Amos; Postilnick, D; Rockah, Rivka; Michaelovsky, Elena; Postilnick, S; Birman, Esther Goldenberg; Laor, Nathaniel; Rauchverger, Boris; Kreinin, Anatoly; Poyurovsky, Michael; Schneidman, Michael; Modai, Ilan; Weizman, Ronit

doi:10.1038/sj.mp.4000536

Cited by 159 publications

(119 citation statements)

References 18 publications

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“…The present observations do not support a major role of the COMT val158met variant in the pathogenesis of major depression, confirming previous findings (Kunugi et al, 1997;Frisch et al, 1999;Cusin et al, 2002;Serretti et al, 2003).…”

Section: Discussionsupporting

confidence: 78%

“…However, the valine allele appears to be less expressed in the brain as compared to the methionine allele (Bray et al, 2003;Zhu et al, 2004), which slightly mitigates the effect to about 40% increased enzyme activity as conferred by the valine allele (Chen et al, 2004). The COMT val158met polymorphism has repeatedly been investigated for association with major depression with contradictory reports of no association (Kunugi et al, 1997;Frisch et al, 1999;Cusin et al, 2002;Serretti et al, 2003), possible association with the valine allele (Massat et al, 2005;Funke et al, 2005) or conversely the methionine allele (Ohara et al, 1998). Two published studies on the role of the COMT val158met polymorphism in antidepressant treatment response investigating samples of 102 and 346 patients, respectively, report a tentative negative effect of the COMT 158met/met genotype on mirtazapine and citalopram response in major depression (Szegedi et al, 2005;Arias et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

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Association of the COMT val158met Variant with Antidepressant Treatment Response in Major Depression

Baune

Hohoff

Berger³

et al. 2007

Neuropsychopharmacol

133

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In several previous biochemical, pharmacological, and genetic studies, the catechol-O-methyltransferase (COMT) has been suggested to be involved in the pathogenesis as well as the pharmacological treatment of affective disorders. In the present study, 256 patients with major depression (DSM-IV) of Caucasian descent were genotyped for the functional COMT val158met polymorphism and characterized for clinical response to antidepressive pharmacological treatment as measured by intra-individual changes of Hamilton Depression (HAM-D-21) scores over 6 weeks. The COMT 158val/val genotype conferred a significant risk of worse response after 4-6 weeks of antidepressant treatment in patients with major depression (week 4: p ¼ 0.003; week 5: po0.0001; week 6: po0.0001) after Bonferroni correction for multiple comparisons. The present results strongly point toward a negative influence of the higher activity COMT 158val/ val genotype on antidepressant treatment response during the first 6 weeks of pharmacological treatment in major depression, possibly conferred by consecutively decreased dopamine availability. This finding suggests a potentially beneficial effect of an antidepressive addon therapy with substances increasing dopamine availability individually tailored according to COMT val158met genotype.

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Section: Discussionsupporting

confidence: 78%

Section: Introductionmentioning

confidence: 99%

Association of the COMT val158met Variant with Antidepressant Treatment Response in Major Depression

Baune

Hohoff

Berger³

et al. 2007

Neuropsychopharmacol

133

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“…Association studies of DRD2 gene polymorphisms and alcoholism or ADHD have suggested that this mechanism might play a role in psychiatric conditions (Comings and MacMurray 2000). However, only one out of eleven other studies investigating the association between 5-HTTLPR and major depression also found that heterozygous subjects are more at risk than the homozygotes, indicating that it is highly unlikely that negative heterosis is present (Bellivier et al 1998;Collier et al 1996;Frisch et al 1999;Furlong et al 1998;Hauser et al 2003;Hoehe et al 1998;Kunugi et al 1997;Mendlewicz et al 2004;Rees et al 1997;Serretti et al 2002;Willis-Owen et al 2005).…”

Section: Discussionmentioning

confidence: 99%

Family Based Association Analyses between the Serotonin Transporter Gene Polymorphism (5-HTTLPR) and Neuroticism, Anxiety and Depression

et al. 2007

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We studied the association between the short/long promotor-based length polymorphism of the serotonin transporter gene (5-HTTLPR) and neuroticism, anxiety and depression. Subjects included twins, their siblings and parents from the Netherlands Twin Register (559 parents and 1,245 offspring). Subjects had participated between one and five times in a survey study measuring neuroticism, anxiety and depression. Offspring of these families were also approached to participate in a psychiatric interview diagnosing DSM-IV major depression. Within-family and total association between 5-HTTLPR and these traits were tested. Only three of the 36 tests showed a significant effect of 5-HTTLPR (P < 0.05). These effects were in opposite directions, i.e. both negative and positive regression coefficients were found for the s allele. No additive effect of the s allele was found for DSM-IV depression. Our results strongly suggest that there is no straightforward association between 5-HTTLPR and neuroticism, anxiety and depression.

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“…Two out of four studies found an increased frequency of the serine variant, indicating that this variant may be associated with major depression (Frisch et al 1999;Lerer et al 2001;Holmes et al 2003;Kö ks et al 2006). 5-HT2C receptor RNA undergoes adenosine-to-inosine RNA modification.…”

Section: -Ht2c Receptormentioning

confidence: 99%

“…5-HT2A receptor polymorphisms are generally not associated with major depression (Zhang et al 1997;Frisch et al 1999;Tsai et al 1999;Minov et al 2001;Oswald et al 2003;Choi et al 2004;Khait et al 2005;Levinson 2005). …”

Section: -Ht Receptorsmentioning

confidence: 99%

Consensus paper of the WFSBP Task Force on Biological Markers: Biological Markers in Depression

Mößner

Mikova

Koutsilieri

et al. 2007

The World Journal of Biological Psychiatry

226

126

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Biological markers for depression are of great interest to aid in elucidating the causes of major depression. We assess currently available biological markers to query their validity for aiding in the diagnosis of major depression. We specifically focus on neurotrophic factors, serotonergic markers, biochemical markers, immunological markers, neuroimaging, neurophysiological findings, and neuropsychological markers. We delineate the most robust biological markers of major depression. These include decreased platelet imipramine binding, decreased 5-HT1A receptor expression, increase of soluble interleukin-2 receptor and interleukin-6 in serum, decreased brain-derived neurotrophic factor in serum, hypocholesterolemia, low blood folate levels, and impaired suppression of the dexamethasone suppression test. To date, however, none of these markers are sufficiently specific to contribute to the diagnosis of major depression. Thus, with regard to new diagnostic manuals such as DSM-V and ICD-11 which are currently assessing whether biological markers may be included in diagnostic criteria, no biological markers for major depression are currently available for inclusion in the diagnostic criteria.

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Association of unipolar major depressive disorder with genes of the serotonergic and dopaminergic pathways

Cited by 159 publications

References 18 publications

Association of the COMT val158met Variant with Antidepressant Treatment Response in Major Depression

Association of the COMT val158met Variant with Antidepressant Treatment Response in Major Depression

Family Based Association Analyses between the Serotonin Transporter Gene Polymorphism (5-HTTLPR) and Neuroticism, Anxiety and Depression

Consensus paper of the WFSBP Task Force on Biological Markers: Biological Markers in Depression

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