Delay in synthesis of the 3 ' splice site promotes trans-splicing of the preceding 5 ' splice site

Takahara T; Tasic B; Maniatis T; Akanuma H; Yanagisawa S

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Delay in synthesis of the 3 ' splice site promotes trans-splicing of the preceding 5 ' splice site

机译：3'剪接位点合成的延迟促进了前面的5'剪接位点的反式剪接

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Premessenger RNA (pre-mRNA) splicing can occur within an individual pre-mRNA (cis-splicing) or between separate pre-mRNAs (trans-spiicing). Although a number of examples of mammalian trans-splicing have been reported, the molecular mechanisms involved are poorly understood. Here, we investigate the mechanisms of Sp1 pre-mRNA trans-splicing with human cells expressing modified Sp1 transgenes. We find that the presence of a long intron or the insertion of an RNA polymerase 11 pause site within an intron promotes trans-splicing. We also add examples of naturally occurring trans-splicing. We propose that Sp1 trans-splicing, and other examples of mammalian trans-splicing, are a consequence of low-frequency disruption of the normal mechanisms that couple transcription and splicing.

机译：前信使RNA（pre-mRNA）剪接可以发生在单个pre-mRNA内（顺式剪接），也可以发生在单独的pre-mRNA之间（反穿刺）。尽管已经报道了许多哺乳动物转拼的例子，但是所涉及的分子机制却知之甚少。在这里，我们调查与人类细胞表达修饰的Sp1转基因的Sp1 pre-mRNA转拼的机制。我们发现长内含子的存在或内含子内RNA聚合酶11暂停位点的插入会促进反式剪接。我们还添加了自然发生的转拼的例子。我们建议Sp1反式剪接，以及其他哺乳动物反式剪接的例子，是对转录和剪接耦合的正常机制进行低频破坏的结果。

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《Molecular cell》 |2005年第2期|共7页
作者
Takahara T; Tasic B; Maniatis T; Akanuma H; Yanagisawa S;
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正文语种 eng
中图分类分子生物学;
关键词
RNA-POLYMERASE-II; SPLICE-SITE SELECTION; MESSENGER-RNA; TRANSCRIPTION ELONGATION; GENE-EXPRESSION; POLYADENYLATION; TERMINATION; PROTEIN; DOMAIN; ALPHA;

机译：RNA聚合酶-Ⅱ;位点选择;信使RNA;转录延伸;基因表达;聚丙烯酰胺化;终止;蛋白质;结构域;α;

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专利

1. Delay in synthesis of the 3 ' splice site promotes trans-splicing of the preceding 5 ' splice site [J] . Takahara T, Tasic B, Maniatis T, Molecular cell . 2005,第2期

机译：3'剪接位点合成的延迟促进了前面的5'剪接位点的反式剪接
2. Minimum free energy predicted base pairing in the 39 nt spliced leader and 5 ' UTR of calmodulin mRNA from Trypanosoma cruzi: influence of the multiple trans-splicing sites [J] . Samudio Franklyn, Brandao Adeilton Anais da Academia Brasileira de Ciências . 2018,第1Suppla2期

机译：来自锥虫瘤Cruzi的39 nt拼接前导植物和5'UTR中的最小自由能量预测基础配对和5'UTR的钙调蛋白mRNA：多逆剪接位点的影响
3. Dysferlin rescue by spliceosome-mediated pre-mRNA trans-splicing targeting introns harbouring weakly defined 3' splice sites [J] . Philippi Susanne, Lorain Stephanie, Beley Cyriaque, Human Molecular Genetics . 2015,第14期

机译：通过剪接体介导的pre-mRNA反式剪接靶向含弱定义的3'剪接位点的内含子来挽救dysferlin
4. Therapeutic Modulation of DMD Splicing by Blocking Exonic Splicing Enhancer Sites with Antisense Oligonucleotides [C] . A.AARTSMA-RUS, A.A.M.JANSON, J.A.HEEMSKERK, Oligonucleotide Therapeutics Society . 2006

机译：用反义寡核苷酸阻断封锁剪接增强剂位点的DMD拼接治疗调节
5. Diverse mechanisms of human genetic disease: Splice order determination in the COL1A2 gene. Effects that influence splice site mutations in osteogenesis imperfecta and a translocation disrupting SNRPN gene causes Prader-Willi syndrome. [D] . Kuslich, Christine D. 1999

机译：人类遗传疾病的多种机制：COL1A2基因的剪接顺序确定。影响成骨不全症中剪接位点突变和易位破坏SNRPN基因的效应会导致Prader-Willi综合征。
6. Intramolecular base pairing between the nematode spliced leader and its 5 splice site is not essential for trans-splicing in vitro. [O] . P A Maroney, G J Hannon, J D Shambaugh, 1991

机译：线虫剪接的前导子与其5剪接位点之间的分子内碱基配对对于体外反式剪接不是必需的。
7. Intramolecular base pairing between the nematode spliced leader and its 5′ splice site is not essential for trans-splicing in vitro. [O] . P.A. Maroney, G.J. Hannon, J.D. Shambaugh, 1991

机译：线虫剪接领导者和其5'剪接部位之间的分子内碱基对对体外抗碎片不是必需的。

Delay in synthesis of the 3 ' splice site promotes trans-splicing of the preceding 5 ' splice site

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