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Alternative polyadenylation confers Pten mRNAs stability and resistance to microRNAs

机译:替代的多腺苷酸化赋予PTEN mRNAS稳定性和抗微大罗氏的耐药性

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摘要

Fine regulation of the phosphatase and tensin homologue (PTEN) phosphatase dosage is critical for homeostasis and tumour suppression. The 3'-untranslated region (3'-UTR) of Pten mRNA was extensively linked to post-transcriptional regulation by microRNAs (miRNAs). In spite of this critical regulatory role, alternative 3'-UTRs of Pten have not been systematically characterized. Here, we reveal an important diversity of Pten mRNA isoforms generated by alternative polyadenylation sites. Several 3'-UTRs are co-expressed and their relative expression is dynamically regulated. In spite of encoding multiple validated miRNA-binding sites, longer isoforms are largely refractory to miRNA-mediated silencing, are more stable and contribute to the bulk of PTEN protein and signalling functions. Taken together, our results warrant a mechanistic re-interpretation of the post-transcriptional mechanisms involving Pten mRNAs and raise concerns on how miRNA-binding sites are being validated.
机译:磷酸酶和张素同源物(PTEN)磷酸酶剂量的细度对于稳态和肿瘤抑制至关重要。 PTEN mRNA的3'-未翻转的区域(3'-UTR)与Micrornas(miRNA)的转录后调节广泛地连接。 尽管存在这种关键的监管作用,但PTEN的替代方案3'-UTR没有系统地表征。 在这里,我们揭示了通过替代多腺苷酸化位点产生的PTEN mRNA同种型的重要多样性。 共同表达几种3'-UTR,并且它们的相对表达是动态调节的。 尽管编码了多个验证的miRNA结合位点,但较长的同种型在很大程度上对miRNA介导的沉默是难以解决的,更稳定并有助于大量PTEN蛋白和信号传导功能。 我们的结果携带,我们的结果是对涉及PTEN MRNA的转录后机制的机械重新解释,并提高对MiRNA结合点的验证方式的担忧。

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