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tRNA-derived fragments and microRNAs in the maternal-fetal interface of a mouse maternal-immune-activation autism model

Zhangli Su, Elizabeth L. Frost, Catherine R. Lammert, Roza Przanowska, John R. Lukens, Anindya Dutta

2020RNA Biology50 citationsDOIOpen Access PDF

Abstract

are abundantly expressed in the normal mouse placenta/decidua. Moreover, tRF and microRNA levels in the maternal-fetal interface change dynamically over the course of embryonic development. To see if stress alters non-coding RNA expression at the maternal-fetal interface, we treated pregnant mice with a viral infection mimetic, which has been shown to promote autism-related phenotypes in the offspring. Acute changes in the levels of specific tRFs and microRNAs were observed 3-6 h after MIA and are suppressed thereafter. A group of 5' tRNA halves is down-regulated by MIA, whereas a group of 18-nucleotide tRF-3a is up-regulated. In conclusion, tRFs show tissue-specificity, developmental changes and acute response to environmental stress, opening the possibility of them having a role in the fetal response to MIA.

Topics & Concepts

BiologyDeciduamicroRNAEpigeneticsFetusPlacentaRNAOffspringSmall RNATransfer RNAGene expressionGeneticsRegulation of gene expressionGenePregnancyRNA modifications and cancerRNA Research and SplicingCancer-related molecular mechanisms research
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