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首页> 外文期刊>Journal of Molecular Biology >UG repeats/TDP-43 interactions near 5′ splice sites exert unpredictable effects on splicing modulation
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UG repeats/TDP-43 interactions near 5′ splice sites exert unpredictable effects on splicing modulation

机译:5'剪接位点附近的UG重复/ TDP-43相互作用对剪接调制产生不可预测的影响

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TDP-43 is a nuclear protein implicated in the pathogenesis of several neurodegenerative diseases such as amyotrophic lateral sclerosis and frontotemporal lobar degeneration, with broad involvement in numerous stages of RNA processing ranging from transcription to translation. In diseased neurons, TDP-43 mostly aggregates in the cytoplasm, suggesting that a loss of protein function in the nucleus may play an important role in neurodegeneration. A better understanding of TDP-43 general nuclear functions is therefore an essential step to evaluate this possibility. Presently, the TDP-43 best-characterized functional property is its ability to modulate pre-mRNA splicing when binding in proximity of 3′SS acceptor sequences. In this work, using a variety of artificial and natural splicing substrates, we have investigated the effects of TDP-43 binding to UG repeats in the vicinity of 5′SS donor sequences. In general, our results show that UG repeats are not powerful splicing regulatory elements when located near to exonic 5′SS sequences. However, in cases like the BRCA1, ETF1, and RXRG genes, TDP-43 binding to natural UG-repeated sequences can act as either an activator or a suppressor of 5′SS recognition, depending on splice site strength and on the presence of additional splicing regulatory sequences. The results of this analysis suggest that a role of UG repeats/TDP-43 in 5′SS recognition may exists and may become critical in the presence of mutations that weaken the 5′SS. The general rule that can be drawn at the moment is that the importance of UG repeats near 5′ splice sites should always be experimentally validated on a case-by-case basis.
机译:TDP-43是一种核蛋白,与多种神经退行性疾病(如肌萎缩性侧索硬化和额颞叶变性)的发病机理有关,广泛参与从转录到翻译的RNA加工的许多阶段。在患病的神经元中,TDP-43主要在细胞质中聚集,这表明细胞核中蛋白质功能的丧失可能在神经变性中起重要作用。因此,更好地了解TDP-43的一般核功能是评估这种可能性的必不可少的步骤。当前,TDP-43最典型的功能特性是当在3'SS受体序列附近结合时,其调节前mRNA剪接的能力。在这项工作中,我们使用各种人工和天然剪接底物,研究了TDP-43与5'SS供体序列附近的UG重复序列结合的作用。通常,我们的结果表明,当位于外显子5'SS序列附近时,UG重复序列不是强大的剪接调控元件。但是,在诸如BRCA1,ETF1和RXRG基因的情况下,与天然UG重复序列结合的TDP-43可以充当5'SS识别的激活剂或抑制剂,具体取决于剪接位点强度和是否存在其他剪接调控序列。该分析的结果表明,UG重复/ TDP-43在5'SS识别中的作用可能存在,并且在弱化5'SS的突变存在下可能变得至关重要。目前可以得出的一般规则是,应始终根据具体情况通过实验验证在5'剪接位点附近UG重复的重要性。

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