Maternal expression of the histone demethylase Kdm4a is crucial for pre-implantation development.

组蛋白甲基化 DNA甲基化 转录因子 染色质重塑
作者
Aditya Sankar,Susanne M. Kooistra,Javier Martin Gonzalez,Claes Ohlsson,Matti Poutanen,Kristian Helin
出处
期刊:Development [The Company of Biologists]
卷期号:144 (18): 3264-3277 被引量:20
标识
DOI:10.1242/dev.155473
摘要

Regulation of chromatin composition through post-translational modifications of histones contributes to transcriptional regulation and is essential for many cellular processes, including differentiation and development. KDM4A (JMJD2A) is a lysine demethylase with specificity towards di- and tri-methylated lysine 9 and lysine 36 of histone H3 (H3K9me2/me3 and H3K36me2/me3). Here, we report that Kdm4a as a maternal factor plays a key role in embryo survival and is vital for female fertility. Kdm4a-/- female mice ovulate normally with comparable fertilization but poor implantation rates, and cannot support healthy transplanted embryos to term. This is due to a role for Kdm4a in uterine function, where its loss causes reduced expression of key genes involved in ion transport, nutrient supply and cytokine signalling, which impact embryo survival. In addition, a significant proportion of Kdm4a-deficient oocytes displays a poor intrinsic ability to develop into blastocysts. These embryos cannot compete with healthy embryos for implantation in vivo, highlighting Kdm4a as a maternal effect gene. Thus, our study dissects an important dual role for maternal Kdm4a in determining faithful early embryonic development and the implantation process.

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