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SRSF7 和 SRSF3 依赖 RNA 测序基序和二级结构来调节 Microprocessor。

SRSF7 and SRSF3 depend on RNA sequencing motifs and secondary structures to regulate Microprocessor.

机构信息

Division of Life Science, The Hong Kong University of Science & Technology, Hong Kong, China.

Division of Life Science, The Hong Kong University of Science & Technology, Hong Kong, China

出版信息

Life Sci Alliance. 2023 Feb 7;6(4). doi: 10.26508/lsa.202201779. Print 2023 Apr.

Abstract

Human Microprocessor cleaves pri-miRNAs to initiate miRNA biogenesis. The accuracy and efficiency of Microprocessor cleavage ensure appropriate miRNA sequence and expression and thus its proper gene regulation. However, Microprocessor cleaves many pri-miRNAs incorrectly, so it requires assistance from many cofactors. For example, SRSF3 enhances Microprocessor cleavage by interacting with the CNNC motif in pri-miRNAs. However, whether SRSF3 can function with other motifs and/or requires the motifs in a certain secondary structure is unknown. In addition, the function of SRSF7 (a paralog of SRSF3) in miRNA biogenesis still needs to be discovered. Here, we demonstrated that SRSF7 could stimulate Microprocessor cleavage. In addition, by conducting high-throughput pri-miRNA cleavage assays for Microprocessor and SRSF7 or SRSF3, we demonstrated that SRSF7 and SRSF3 function with the CRC and CNNC motifs, adopting certain secondary structures. In addition, SRSF7 and SRSF3 affect the Microprocessor cleavage sites in human cells. Our findings demonstrate the roles of SRSF7 in miRNA biogenesis and provide a comprehensive view of the molecular mechanism of SRSF7 and SRSF3 in enhancing Microprocessor cleavage.

摘要

人类微处理器切割 pri-miRNAs 以启动 miRNA 生物发生。微处理器切割的准确性和效率确保了适当的 miRNA 序列和表达,从而实现了适当的基因调控。然而,微处理器错误地切割了许多 pri-miRNAs,因此它需要许多辅助因子的帮助。例如,SRSF3 通过与 pri-miRNAs 中的 CNNC 基序相互作用增强微处理器切割。然而,SRSF3 是否可以与其他基序一起发挥作用,或者是否需要特定的二级结构中的基序尚不清楚。此外,SRSF7(SRSF3 的同源物)在 miRNA 生物发生中的功能仍有待发现。在这里,我们证明了 SRSF7 可以刺激微处理器切割。此外,通过进行 Microprocessor 和 SRSF7 或 SRSF3 的高通量 pri-miRNA 切割分析,我们证明了 SRSF7 和 SRSF3 与 CRC 和 CNNC 基序一起作用,采用特定的二级结构。此外,SRSF7 和 SRSF3 影响人类细胞中的 Microprocessor 切割位点。我们的发现证明了 SRSF7 在 miRNA 生物发生中的作用,并提供了 SRSF7 和 SRSF3 增强微处理器切割的分子机制的全面视图。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b5ff/9905709/5d076242fc51/LSA-2022-01779_Fig1.jpg

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