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  Genome-wide gene expression changes in postpartum depression point towards an altered immune landscape

Mehta, D., Grewen, K., Pearson, B., Wani, S., Wallace, L., Henders, A. K., et al. (2021). Genome-wide gene expression changes in postpartum depression point towards an altered immune landscape. TRANSLATIONAL PSYCHIATRY, 11(1): 155. doi:10.1038/s41398-021-01270-5.

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 Creators:
Mehta, Divya, Author
Grewen, Karen, Author
Pearson, Brenda, Author
Wani, Shivangi, Author
Wallace, Leanne, Author
Henders, Anjali K., Author
Binder, Elisabeth B.1, Author           
Frokjaer, Vibe G., Author
Meltzer-Brody, Samantha, Author
Wray, Naomi R., Author
Stuebe, Alison M., Author
Affiliations:
1Dept. Translational Research in Psychiatry, Max Planck Institute of Psychiatry, Max Planck Society, ou_2035295              

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 Abstract: Maternal postpartum depression (PPD) is a significant public health concern due to the severe negative impact on maternal and child health and well-being. In this study, we aimed to identify genes associated with PPD. To do this, we investigated genome-wide gene expression profiles of pregnant women during their third trimester of pregnancy and tested the association of gene expression with perinatal depressive symptoms. A total of 137 women from a cohort from the University of North Carolina, USA were assessed. The main phenotypes analysed were Edinburgh Postnatal Depression Scale (EPDS) scores at 2 months postpartum and PPD (binary yes/no) based on an EPDS cutoff of 10. Illumina NextSeq500/550 transcriptomic sequencing from whole blood was analysed using the edgeR package. We identified 71 genes significantly associated with postpartum depression scores at 2 months, after correction for multiple testing at 5% FDR. These included several interesting candidates including TNFRSF17, previously reported to be significantly upregulated in women with PPD and MMP8, a matrix metalloproteinase gene, associated with depression in a genome-wide association study. Functional annotation of differentially expressed genes revealed an enrichment of immune response-related biological processes. Additional analysis of genes associated with changes in depressive symptoms from recruitment to 2 months postpartum identified 66 genes significant at an FDR of 5%. Of these genes, 33 genes were also associated with depressive symptoms at 2 months postpartum. Comparing the results with previous studies, we observed that 15.4% of genes associated with PPD in this study overlapped with 700 core maternal genes that showed significant gene expression changes across multiple brain regions (P = 7.9e-05) and 29-53% of the genes were also associated with estradiol changes in a pharmacological model of depression (P values range = 1.2e-4-2.1e-14). In conclusion, we identified novel genes and validated genes previously associated with oestrogen sensitivity in PPD. These results point towards the role of an altered immune transcriptomic landscape as a vulnerability factor for PPD.

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 Dates: 2021
 Publication Status: Published online
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Title: TRANSLATIONAL PSYCHIATRY
Source Genre: Journal
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Pages: - Volume / Issue: 11 (1) Sequence Number: 155 Start / End Page: - Identifier: ISSN: 2158-3188