The methyltransferase complex (MTC) deposits N6-adenosine (m(6)A) onto RNA, whereas the microprocessor produces microRNA. Whether and how these two distinct complexes cross-regulate each other has been poorly studied. Here we report that the MTC subunit B tends to form insoluble condensates with poor activity, with its level monitored by the 20S proteasome. Conversely, the microprocessor component SERRATE (SE) forms liquid-like condensates, which in turn promote the solubility and stability of the MTC subunit B, leading to increased MTC activity. Consistently, the hypomorphic lines expressing SE variants, defective in MTC interaction or liquid-like phase behaviour, exhibit reduced m(6)A levels. Reciprocally, MTC can recruit the microprocessor to the MIRNA loci, prompting co-transcriptional cleavage of primary miRNA substrates. Additionally, primary miRNA substrates carrying m(6)A modifications at their single-stranded basal regions are enriched by m(6)A readers, which retain the microprocessor in the nucleoplasm for continuing processing. This reveals an unappreciated mechanism of phase separation in RNA modification and processing through MTC and microprocessor coordination.
SERRATE drives phase separation behaviours to regulate m6A modification and miRNA biogenesis.
SERRATE 驱动相分离行为以调节 m6A 修饰和 miRNA 生物合成
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作者:Zhong Songxiao, Li Xindi, Li Changhao, Bai Haiyan, Chen Jingjing, Gan Lu, Zhu Jiyun, Oh Taerin, Yan Xingxing, Zhu Jiaying, Li Niankui, Koiwa Hisashi, Meek Thomas, Peng Xu, Yu Bin, Zhang Zhonghui, Zhang Xiuren
| 期刊: | Nature Cell Biology | 影响因子: | 19.100 |
| 时间: | 2024 | 起止号: | 2024 Dec;26(12):2129-2143 |
| doi: | 10.1038/s41556-024-01530-8 | 研究方向: | 其它 |
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