Study Report
Reference
Citation | Laje, 2010 PubMed |
Full Info | Laje, G., Cannon, D.M., Allen, A.S., Klaver, J.M., Peck, S.A., Liu, X., Manji, H.K., Drevets, W.C. and McMahon, F.J. (2010) Genetic variation in HTR2A influences serotonin transporter binding potential as measured using PET and [11C]DASB. Int J Neuropsychopharmacol, 13, 715-724.
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Study
Hypothesis or Background |
In a previous study we showed that genetic variation in HTR2A, which encodes the serotonin 2A receptor, influenced outcome of citalopram treatment in patients with major depressive disorder. Since chronic administration of citalopram, which selectively and potently inhibits the serotonin transporter (5-HTT), putatively enhances serotonergic transmission, it is conceivable that genetic variation within HTR2A also influences pretreatment 5-HTT function or serotonergic transmission. The present study used positron emission tomography (PET) and the selective 5-HTT ligand, [11C]DASB, to investigate whether the HTR2A marker alleles that predict treatment outcome also predict differences in 5-HTT binding.
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Sample Information | 43 patients and healthy volunteers |
Method Detail | Brain levels of 5-HTT were assessed in vivo using PET measures of the non-displaceable component of the [11C]DASB binding potential (BPND). DNA from 43 patients and healthy volunteers, all unmedicated, was genotyped with 14 single nucleotide polymorphisms located within or around HTR2A. Allelic association with BPND was assessed in eight brain regions, with covariates to control for race and ethnicity. We detected allelic association between [11C]DASB BPND in thalamus and three markers in a region spanning the 3' untranslated region and second intron of HTR2A (rs7333412, p=0.000045; rs7997012, p=0.000086; rs977003, p=0.000069). |
Method Keywords | positron emission tomography (PET); genotyping |
Result | The association signal at rs7333412 remained significant (p<0.05) after applying corrections for multiple testing via permutation. Genetic variation in HTR2A that was previously associated with citalopram treatment outcome was also associated with thalamic 5-HTT binding. |
Conclusions | While further work is needed to identify the actual functional genetic variants involved, these results suggest that a relationship exists between genetic variation in HTR2A and either 5-HTT expression or central serotonergic transmission that influences the therapeutic response to 5-HTT inhibition in major depression. |
Relationships reported by
Laje, 2010
Component A Approved Name (Name in Paper) |
Component A Type |
Component B Approved Name (Name in Paper) |
Component B Type |
Statistical Result |
Relationship Description |
Result Category (Positive/Negative)) |
Sodium-dependent serotonin transporter (serotonin transporter (5-HTT))
|
protein |
HTR2A (HTR2A) |
gene |
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Genetic variation in HTR2A that was previously associated with citalopram treatment outcome was also associated with thalamic 5-HTT binding. |
Positive
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MDD
|
syndrome |
rs7333412 (rs7333412) |
SNP |
P-value<0.05 |
The association signal at rs7333412 remained significant (p<0.05) after applying corrections for multiple testing via permutation. |
Positive
|
Thalamus (thalamus)
|
brain morphology and function |
HTR2A (HTR2A) |
gene |
|
Genetic variation in HTR2A that was previously associated with citalopram treatment outcome was also associated with thalamic 5-HTT binding. |
Positive
|