The spliceosome executes pre-mRNA splicing through four sequential stages: assembly, activation, catalysis, and disassembly. Activation of the spliceosome, namely remodeling of the pre-catalytic spliceosome (B complex) into the activated spliceosome (B(act) complex) and the catalytically activated spliceosome (B(*) complex), involves major flux of protein components and structural rearrangements. Relying on a splicing inhibitor, we have captured six intermediate states between the B and B(*) complexes: pre-B(act), B(act)-I, B(act)-II, B(act)-III, B(act)-IV, and post-B(act). Their cryo-EM structures, together with an improved structure of the catalytic step I spliceosome (C complex), reveal how the catalytic center matures around the internal stem loop of U6 snRNA, how the branch site approaches 5'-splice site, how the RNA helicase PRP2 rearranges to bind pre-mRNA, and how U2 snRNP undergoes remarkable movement to facilitate activation. We identify a previously unrecognized key role of PRP2 in spliceosome activation. Our study recapitulates a molecular choreography of the human spliceosome during its catalytic activation.
Molecular basis for the activation of human spliceosome.
人类剪接体激活的分子基础
阅读:12
作者:Zhan Xiechao, Lu Yichen, Shi Yigong
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2024 | 起止号: | 2024 Jul 27; 15(1):6348 |
| doi: | 10.1038/s41467-024-50785-0 | 种属: | Human |
| 研究方向: | 其它 | ||
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