Maternal RNA Transcription in Dlk1-Dio3 Domain is Critical for Proper Development of the Mouse Placental Vasculature

Overview

Journal Commun Biol

Specialty Biology

Date 2024 Mar 24

PMID 38521877

Authors

Ximeijia Zhang

Hongjuan He

Haoran Yu

Xiangqi Teng

Ziwen Wang

Chenghao Li

Jiahang Li

Haopeng Yang

Jiwei Shen

Tong Wu

Fengwei Zhang

Yan Zhang

Qiong Wu

Affiliations

Soon will be listed here.

Abstract

The placenta is a unique organ for ensuring normal embryonic growth in the uterine. Here, we found that maternal RNA transcription in Dlk1-Dio3 imprinted domain is essential for placentation. PolyA signals were inserted into Gtl2 to establish a mouse model to prevent the expression of maternal RNAs in the domain. The maternal allele knock-in (MKI) and homozygous (HOMO) placentas showed an expanded junctional zone, reduced labyrinth and poor vasculature impacting both fetal and maternal blood spaces. The MKI and HOMO models displayed dysregulated gene expression in the Dlk1-Dio3 domain. In situ hybridization detected Dlk1, Gtl2, Rtl1, miR-127 and Rian dysregulated in the labyrinth vasculature. MKI and HOMO induced Dlk1 to lose imprinting, and DNA methylation changes of IG-DMR and Gtl2-DMR, leading to abnormal gene expression, while the above changes didn't occur in paternal allele knock-in placentas. These findings demonstrate that maternal RNAs in the Dlk1-Dio3 domain are involved in placental vasculature, regulating gene expression, imprinting status and DNA methylation.

Citing Articles

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