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BMI1 promotes spermatogonial stem cell maintenance by epigenetically repressing Wnt10b/β-catenin signaling

Jun Yu, Cong Shen, Meng Lin, Xia Chen, Xiuliang Dai, Zhiran Li, Yunhao Wu, Yangbo Fu, Jinxing Lv, Xiaoyan Huang, Bo Zheng, Fei Sun

2022International Journal of Biological Sciences28 citationsDOIOpen Access PDF

Abstract

The self-renewal of spermatogonial stem cells (SSCs) requires a special microenvironment and is strictly controlled. Previously, we identified BMI1 as a key regulator of spermatogenesis in a knock-out mouse model. However, the mechanisms by which BMI1 regulates SSC maintenance remain largely unknown. Herein, we show that BMI1 is essential for SSC maintenance. BMI1 directs the transcriptional repression of target genes by increasing H2AK119ub and reducing H3K4me3 in SSCs. Furthermore, BMI1 inhibition resulted in the transcriptional activation of Wnt10b and thereby promoted the nuclear translocation of -catenin in SSCs. Importantly, the suppression of Wnt/-catenin signaling restored both the cytoplasmic expression of -catenin and SSC maintenance in BMI1-deficient SSCs. Finally, we demonstrated that Wnt/-catenin signaling was also involved in BMI1-mediated SSC maintenance in vivo. Altogether, our study not only reveals a novel mechanism for BMI1 in the process of SSC maintenance, but also provides a potential new strategy for treating male infertility.

Topics & Concepts

BMI1Wnt signaling pathwayPsychological repressionBiologyCell biologyStem cellH3K4me3CateninSignal transductionRegulatorCancer researchBeta-cateninPromoterGeneticsGeneGene expressionSperm and Testicular FunctionReproductive Biology and FertilityGenetic and Clinical Aspects of Sex Determination and Chromosomal Abnormalities
BMI1 promotes spermatogonial stem cell maintenance by epigenetically repressing Wnt10b/β-catenin signaling | Litcius