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HDAC6 regulates primordial follicle activation through mTOR signaling pathway
Tuo Zhang, Meina He, Lihua Zhao, Shaogang Qin, Zijian Zhu, Xinhua Du, Bo Zhou, Yi Yang, Xinfeng Liu, Guoliang Xia, Tengxiang Chen, Yuanxi Wang, Hua Zhang, Chao Wang
Cell Death and Disease · 2021 · ▲ 61 citations
Epigenetic alterations
Deregulated nutrient-sensing
Altered intercellular communication
Cell culture / in vitro
Mouse
In vitro
Abstract
Primordial follicle pool established perinatally is a non-renewable resource which determines the female fecundity in mammals. While the majority of primordial follicles in the primordial follicle pool maintain dormant state, only a few of them are activated into growing follicles in adults in each cycle. Excessive activation of the primordial follicles accelerates follicle pool consumption and leads to premature ovarian failure. Although previous studies including ours have emphasized the importance of keeping the balance between primordial follicle activation and dormancy via molecules within the primordial follicles, such as TGF-β, E-Cadherin, mTOR(definition), and AKT through different mechanisms, the homeostasis regulatory mechanisms of primordial follicle activation remain unclear. Here, we reported that HDAC6 acts as a key negative regulator of mTOR in dormant primordial follicles. In the cytoplasm of both oocytes and granulosa cells of primordial follicles, HDAC6 expressed strong, however in those activated primordial follicles, its expression level is relatively weaker. Inhibition or knockdown of HDAC6 significantly promoted the activation of limited primordial follicles while the size of follicle pool was not affected profoundly in vitro. Importantly, the expression level of mTOR in the follicle and the activity of PI3K in the oocyte of the follicle were simultaneously up-regulated after inhibiting of HDAC6. The up-regulated mTOR leads to not only the growth and differentiation of primordial follicles granulosa cells (pfGCs) into granulosa cells (GCs), but the increased secretion of KITL in these somatic cells. As a result, inhibition of HDAC6 awaked the dormant primordial follicles of mice in vitro. In conclusion, HDAC6 may play an indispensable role in balancing the maintenance and activation of primordial follicles through mTOR signaling in mice. These findings shed new lights on uncovering the epigenetic factors involved physiology of sustaining female reproduction.
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- DOI
- 10.1038/s41419-021-03842-1
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- 2026-06-13 MST
Cite this
APA
Zhang, T., He, M., Zhao, L., Qin, S., Zhu, Z., Du, X., Zhou, B., Yang, Y., Liu, X., Xia, G., Chen, T., Wang, Y., Zhang, H., & Wang, C. (2021). HDAC6 regulates primordial follicle activation through mTOR signaling pathway. <em>Cell Death and Disease</em>. https://doi.org/10.1038/s41419-021-03842-1
Vancouver
Zhang T, He M, Zhao L, Qin S, Zhu Z, Du X, et al. HDAC6 regulates primordial follicle activation through mTOR signaling pathway. Cell Death and Disease. 2021. doi:10.1038/s41419-021-03842-1.
BibTeX
@article{tuo2021HDACre,
title = {HDAC6 regulates primordial follicle activation through mTOR signaling pathway},
author = {Tuo Zhang and Meina He and Lihua Zhao and Shaogang Qin and Zijian Zhu and Xinhua Du and Bo Zhou and Yi Yang and Xinfeng Liu and Guoliang Xia and Tengxiang Chen and Yuanxi Wang and Hua Zhang and Chao Wang},
journal = {Cell Death and Disease},
year = {2021},
doi = {10.1038/s41419-021-03842-1},
}
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