Chromatin Modifier EP400 Regulates Oocyte Quality and Zygotic Genome Activation in Mice

Overview

Journal Adv Sci (Weinh)

Specialty Biomedical Engineering

Date 2024 Mar 17

PMID 38493496

Authors

Qing Tian

Ying Yin

Yu Tian

Yufan Wang

Yong-Feng Wang

Rikiro Fukunaga

Toshihiro Fujii

Ai-Hua Liao

Lei Li

Wei Zhang

Ximiao He

Wenpei Xiang

Li-Quan Zhou

Affiliations

Soon will be listed here.

Abstract

Epigenetic modifiers that accumulate in oocytes, play a crucial role in steering the developmental program of cleavage embryos and initiating life. However, the identification of key maternal epigenetic regulators remains elusive. In the findings, the essential role of maternal Ep400, a chaperone for H3.3, in oocyte quality and early embryo development in mice is highlighted. Depletion of Ep400 in oocytes resulted in a decline in oocyte quality and abnormalities in fertilization. Preimplantation embryos lacking maternal Ep400 exhibited reduced major zygotic genome activation (ZGA) and experienced developmental arrest at the 2-to-4-cell stage. The study shows that EP400 forms protein complex with NFYA, occupies promoters of major ZGA genes, modulates H3.3 distribution between euchromatin and heterochromatin, promotes transcription elongation, activates the expression of genes regulating mitochondrial functions, and facilitates the expression of rate-limiting enzymes of the TCA cycle. This intricate process driven by Ep400 ensures the proper execution of the developmental program, emphasizing its critical role in maternal-to-embryonic transition.

Citing Articles

The impact of retrotransposons on zygotic genome activation and the chromatin landscape of early embryos.

Solberg T, Kobayashi-Ishihara M, Siomi H Ann N Y Acad Sci. 2024; 1542(1):11-24.

PMID: 39576233 PMC: 11668504. DOI: 10.1111/nyas.15260.

Chromatin Modifier EP400 Regulates Oocyte Quality and Zygotic Genome Activation in Mice.

Tian Q, Yin Y, Tian Y, Wang Y, Wang Y, Fukunaga R Adv Sci (Weinh). 2024; 11(20):e2308018.

PMID: 38493496 PMC: 11132066. DOI: 10.1002/advs.202308018.

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