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Mutagenesis of Snu114 domain IV identifies a developmental role in meiotic splicing

机译:SNU114结构域IV的诱变鉴定了减数分裂拼接的发育作用

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摘要

Snu114, a component of the U5 snRNP, plays a key role in activation of the spliceosome. It controls the action of Brr2, an RNA-stimulated ATPase/RNA helicase that disrupts U4/U6 snRNA base-pairing prior to formation of the spliceosome's catalytic centre. Snu114 has a highly conserved domain structure that resembles that of the GTPase EF-2/EF-G in the ribosome. It has been suggested that the regulatory function of Snu114 in activation of the spliceosome is mediated by its C-terminal region, however, there has been only limited characterisation of the interactions of the C-terminal domains. We show a direct interaction between protein phosphatase PP1 and Snu114 domain 'IVa' and identify sequence 'YGVQYK' as a PP1 binding motif. Interestingly, this motif is also required for Cwc21 binding. We provide evidence for mutually exclusive interaction of Cwc21 and PP1 with Snu114 and show that the affinity of Cwc21 and PP1 for Snu114 is influenced by the different nucleotide-bound states of Snu114. Moreover, we identify a novel mutation in domain IVa that, while not affecting vegetative growth of yeast cells, causes a defect in splicing transcripts of the meiotic genes, SPO22, AMA1 and MER2, thereby inhibiting an early stage of meiosis.
机译:SNU114是U5 SNRNP的组成部分在激活抗乳头体中起着关键作用。它控制BRR2,RNA刺激的ATP酶/ RNA螺旋酶的作用,其在形成抗磷酸体催化中心之前破坏U4 / U6 SnRNA碱基配对。 SNU114具有高度保守的域结构,其类似于核糖体中GTP酶EF-2 / EF-G的结构。已经提出,SNU114在激活抗乳头组中的调节功能由其C末端区域介导,然而,仅有限的C末端结构域的相互作用表征。我们展示了蛋白质磷酸酶PP1和SNU114结构域'IVA'之间的直接相互作用,并鉴定序列'YGVQyk'作为PP1结合基序。有趣的是,CWC21绑定也需要该基序。我们提供CWC21和PP1与SNU114相互排他性相互作用的证据,并表明CWC21和PP1对SNU114的亲和力受SNU114的不同核苷酸结合状态的影响。此外,我们鉴定域IVA中的新突变,同时不影响酵母细胞的营养生长,导致减数基因,SPO22,AMA1和MER2的剪接转录物的缺陷,从而抑制减数分裂的早期阶段。

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