4.7 Article

Identification and functional characterization of the extremely long allele of the serotonin transporter-linked polymorphic region

TRANSLATIONAL PSYCHIATRY (2021)

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Journal

TRANSLATIONAL PSYCHIATRY
Volume 11, Issue 1, Pages -

Publisher

SPRINGERNATURE
DOI: 10.1038/s41398-021-01242-9

Keywords

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Categories

Psychiatry

Funding

  1. Japan Society for the Promotion of Science KAKENHI [16H06395, 16H06399, 16K21720, 18H02753, 18H05428, 18H05430, 18H05435, 18K07567, 19K17056]
  2. AMED [JP20dm0107097, JP20km0405201, JP20km0405208, JP20dm0107123, JP20dm0207074, JP20dk0207025, JP20dm0307001, JP20dm0307004, JP20dm0207069]
  3. UTokyo Center for Integrative Science of Human Behavior(CiSHuB)
  4. International Research Center for Neurointelligence (WPI-IRCN) at The University of Tokyo Institutes for Advanced Study (UTIAS)
  5. Grants-in-Aid for Scientific Research [19K17056, 18K07567, 18H05430, 18H02753] Funding Source: KAKEN

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The study identifies a novel 5-HTTLPR allele, XL28-A, in the Japanese population and suggests that it is unlikely to be associated with psychiatric disorders, despite its functional deficit. This highlights the importance of unraveling the complex genetic variations of 5-HTTLPR for further understanding its role in psychiatric disorders.
SLC6A4, which encodes the serotonin transporter, has a functional polymorphism called the serotonin transporter-linked polymorphic region (5-HTTLPR). The 5-HTTLPR consists of short (S) and long (L) alleles, each of which has 14 or 16 tandem repeats. In addition, the extralong (XL) and other rare alleles have been reported in 5-HTTLPR. Although they are more frequent in Asian and African than in other populations, the extent of variations and allele frequencies (AFs) were not addressed in a large population. Here, we report the AFs of the rare alleles in a large number of Japanese subjects (N=2894) consisting of two cohorts. The first cohort (case-control study set, CCSS) consisted of 1366 subjects, including 485 controls and 881 patients with psychosis (bipolar disorder or schizophrenia). The second cohort (the Arao cohort study set, ACSS) consisted of 1528 elderly subjects. During genotyping, we identified 11 novel 5-HTTLPR alleles, including 3 XL alleles. One novel allele had the longest subunit ever reported, consisting of 28 tandem repeats. We named this XL28-A. An in vitro luciferase assay revealed that XL28-A has no transcriptional activity. XL28-A was found in two unrelated patients with bipolar disorder in the CCSS and one healthy subject in the ACSS who did not show depressive symptoms or a decline in cognitive function. Therefore, it is unlikely that XL28-A is associated with psychiatric disorders, despite its apparent functional deficit. Our results suggest that unraveling the complex genetic variations of 5-HTTLPR will be important for further understanding its role in psychiatric disorders.

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