Epigenetics of the molecular clock and bacterial diversity in bipolar disorder.


Journal

Psychoneuroendocrinology
ISSN: 1873-3360
Titre abrégé: Psychoneuroendocrinology
Pays: England
ID NLM: 7612148

Informations de publication

Date de publication:
03 2019
Historique:
received: 04 07 2018
revised: 04 11 2018
accepted: 06 11 2018
pubmed: 23 11 2018
medline: 4 3 2020
entrez: 23 11 2018
Statut: ppublish

Résumé

Objectives The gut microbiome harbors substantially more genetic material than our body cells and has an impact on a huge variety of physiological mechanisms including the production of neurotransmitters and the interaction with brain functions through the gut-brain-axis. Products of microbiota can affect methylation according to preclinical studies. The current investigation aimed at analyzing the correlation between gut microbiome diversity and the methylation of the clock gene ARNTL in individuals with Bipolar Disorder (BD). Methods Genomic DNA was isolated from fasting blood of study participants with BD (n = 32). The methylation analysis of the ARNTL CG site cg05733463 was performed by bisulfite treatment of genomic DNA with the Epitect kit, PCR and pyrosequencing. Additionally, DNA was extracted from stool samples and subjected to 16S rRNA sequencing. QIIME was used to analyze microbiome data. Results Methylation status of the ARNTL CpG position cg05733463 correlated significantly with bacterial diversity (Simpson index: r= -0.389, p =  0.0238) and evenness (Simpson evenness index: r= -0.358, p =  0.044). Furthermore, bacterial diversity differed significantly between euthymia and depression (F(1,30) = 4.695, p =  0.039). Discussion The results of our pilot study show that bacterial diversity differs between euthymia and depression. Interestingly, gut microbiome diversity and evenness correlate negatively with methylation of ARNTL, which is known to regulate monoamine oxidase A transcription. We propose that alterations in overall diversity of the gut microbiome represent an internal environmental factor that has an epigenetic impact on the clock gene ARNTL which is thought to be involved in BD pathogenesis.

Identifiants

pubmed: 30465968
pii: S0306-4530(18)30674-7
doi: 10.1016/j.psyneuen.2018.11.009
pii:
doi:

Substances chimiques

ARNTL Transcription Factors 0
BMAL1 protein, human 0
RNA, Ribosomal, 16S 0

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

160-166

Informations de copyright

Copyright © 2018. Published by Elsevier Ltd.

Auteurs

S A Bengesser (SA)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

S Mörkl (S)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria. Electronic address: sabrina.moerkl@medunigraz.at.

A Painold (A)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

N Dalkner (N)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

A Birner (A)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

F T Fellendorf (FT)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

M Platzer (M)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

R Queissner (R)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

C Hamm (C)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

A Maget (A)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

R Pilz (R)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

A Rieger (A)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

J Wagner-Skacel (J)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

B Reininghaus (B)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

H P Kapfhammer (HP)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

E Petek (E)

MUG, Diagnostic & Research Institute of Human Genetics, Austria.

K Kashofer (K)

MUG, Institute of Pathology, Austria.

B Halwachs (B)

MUG, Institute of Pathology, Austria.

P Holzer (P)

MUG, Otto Loewi Research Centre, Austria.

A Waha (A)

University of Bonn, Institute of Neuropathology, Germany.

E Z Reininghaus (EZ)

Medical University of Graz (MUG), Department of Psychiatry and Psychotherapeutic Medicine, Austria.

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Classifications MeSH