Literature DB >> 31284290

Association of childhood traumatization and neuropsychiatric outcomes with altered plasma micro RNA-levels.

Sandra Van der Auwera1,2, Sabine Ameling3,4, Katharina Wittfeld5,6, Enrique d'Harcourt Rowold5, Matthias Nauck4,7, Henry Völzke4,8, Karsten Suhre9, Hani Najafi-Shoushtari10,11, Jaicy Methew11, Vimal Ramachandran11, Robin Bülow12, Uwe Völker3,4, Hans J Grabe5,6.   

Abstract

Childhood traumatization (CT) is associated with the development of several neuropsychiatric disorders in later life. Experimental data in animals and observational data in humans revealed evidence for biological alterations in response to CT that may contribute to its long-term consequences. This includes epigenetic changes in miRNA levels that contribute to complex alterations of gene expression. We investigated the association between CT and 121 miRNAs in a target sample of N = 150 subjects from the general population and patients from the Department of Psychiatry. We hypothesized that CT exhibits a long-term effect on miRNA plasma levels. We supported our findings using bioinformatics tools and databases. Among the 121 miRNAs 22 were nominally significantly associated with CT and four of them (let-7g-5p, miR-103a-3p, miR-107, and miR-142-3p) also after correction for multiple testing; most of them were previously associated with Alzheimer's disease (AD) or depression. Pathway analyses of target genes identified significant pathways involved in neurodevelopment, inflammation and intracellular transduction signaling. In an independent general population sample (N = 587) three of the four miRNAs were replicated. Extended analyses in the general population sample only (N = 687) showed associations of the four miRNAs with gender, memory, and brain volumes. We gained increasing evidence for a link between CT, depression and AD through miRNA alterations. We hypothesize that depression and AD not only share environmental factors like CT but also biological factors like altered miRNA levels. This miRNA pattern could serve as mediating factor on the biological path from CT to adult neuropsychiatric disorders.

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Year:  2019        PMID: 31284290      PMCID: PMC6898678          DOI: 10.1038/s41386-019-0460-2

Source DB:  PubMed          Journal:  Neuropsychopharmacology        ISSN: 0893-133X            Impact factor:   7.853


  48 in total

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