Genetic variation in the serotonin transporter promoter region affects serotonin uptake in human blood platelets

Greenberg, Benjamin D.; Tolliver, Teresa J.; Huang, Su‐Jan; Li, Qian; Bengel, Dietmar; Murphy, Dennis L.

doi:10.1002/(sici)1096-8628(19990205)88:1<83::aid-ajmg15>3.3.co;2-s

Cited by 200 publications

(270 citation statements)

References 11 publications

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“…These findings are in accordance with functional effects on higher platelet serotonin uptake mediated by the long allele variants of 5HTTLPR in healthy controls. 229 No difference was found between genotypes for whole-blood serotonin levels in two samples of individuals with AD, 236,245 which parallels the findings in healthy controls.…”

Section: Chromosome 17supporting

confidence: 57%

“…The most common assessed variants are a deletion/ insertion polymorphism in the transcriptional control region of the SLC6A4 gene with functional effects (5HTTLPR) [227][228][229] and a variable number of tandem repeat in intron 2 (STin2). Several studies have found an association of the short alleles of 5HTTLPR with AD, 217,[230][231][232][233] fewer studies of the long alleles.…”

Section: Chromosome 17mentioning

confidence: 99%

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The genetics of autistic disorders and its clinical relevance: a review of the literature

2006

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Twin and family studies in autistic disorders (AD) have elucidated a high heritability of the narrow and broad phenotype of AD. In this review on the genetics of AD, we will initially delineate the phenotype of AD and discuss aspects of differential diagnosis, which are particularly relevant with regard to the genetics of autism. Cytogenetic and molecular genetic studies will be presented in detail, and the possibly involved aetiopathological pathways will be described. Implications of the different genetic findings for genetic counselling will be mentioned.

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Section: Chromosome 17supporting

confidence: 57%

Section: Chromosome 17mentioning

confidence: 99%

The genetics of autistic disorders and its clinical relevance: a review of the literature

2006

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“…68,[70][71][72][73] However, the translation of in vitro findings into in vivo functioning does not appear straightforward. Human neuroimaging studies of 5-HTT availability [74][75][76][77][78][79] and post-mortem studies of 5-HTT bindings and rRNA expression [80][81][82] have not detected any consistent effect of 5-HTTLPR. No reliable association was found between 5-HTLPR and the level of serotonin metabolite in the cerebrospinal fluid.…”

Section: The Functionality Of 5-httlprmentioning

confidence: 99%

The moderation by the serotonin transporter gene of environmental adversity in the aetiology of mental illness: review and methodological analysis

2007

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“…39,38 Serotonin transporter function has been characterized in platelets using [ 3 H]-serotonin with typical K m values reported in the nano-to micromolar range. 19,40 Lymphocyte SERT 30,41 and DAT 42,43 expression have also recently been described. Serotonin transporters are reported to be expressed in primary B-lymphocytes, 41 T-lymphocytes, 41 and mixed lymphocyte populations.…”

mentioning

confidence: 96%

“…Serotonin transporter regulation and function have been studied using radiometric assay, voltammetry, or fluorescence microscopy in synaptosomes, 16−18 platelets, 19,20 peripheral blood cells (PBCs), 21,22 lymphoblasts, 23−25 brain slices, 1 and the intact brains of experimental animals. [26][27][28]2 Although SERT function can be effectively measured by all of these methods, ambiguity arises when samples containing multiple cell types, such as PBCs, are investigated due to the difficulty in assigning uptake to individual cell types.…”

mentioning

confidence: 99%

Serotonin Uptake Is Largely Mediated by Platelets versus Lymphocytes in Peripheral Blood Cells

Beikmann

Tomlinson²,

Rosenthal³

et al. 2012

ACS Chem. Neurosci.

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ABSTRACT:The serotonin transporter (SERT), a primary target for many antidepressants, is expressed in the brain and also in peripheral blood cells. Although platelet SERT function is well accepted, lymphocyte SERT function has not been definitively characterized. Due to their small size, platelets often are found in peripheral blood mononuclear cell preparations aimed at isolating lymphocytes, monocytes, and macrophages. The presence of different cells makes it difficult to assign SERT expression and function to specific cell types. Here, we use flow cytometry and IDT307, a monoamine transporter substrate that fluoresces after uptake into cells, to investigate SERT function in lymphocyte and platelet populations independently, as well as simultaneously without prior isolation. We find that murine lymphocytes exhibit temperature-dependent IDT307 transport but uptake is independent of SERT. Lack of measurable SERT function in lymphocytes was corroborated by chronoamperometry using serotonin as a substrate. When we examined rhesus and human mixed blood cell populations, we found that platelets, and not lymphocytes, were primary contributors to SERT function. Overall, these findings indicate that lymphocyte SERT function is minimal. Moreover, flow cytometry, in conjunction with the fluorescent transporter substrate IDT307, can be widely applied to investigate SERT in platelets from populations of clinical significance.

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Genetic variation in the serotonin transporter promoter region affects serotonin uptake in human blood platelets

Cited by 200 publications

References 11 publications

The genetics of autistic disorders and its clinical relevance: a review of the literature

The genetics of autistic disorders and its clinical relevance: a review of the literature

The moderation by the serotonin transporter gene of environmental adversity in the aetiology of mental illness: review and methodological analysis

Serotonin Uptake Is Largely Mediated by Platelets versus Lymphocytes in Peripheral Blood Cells

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