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Co-occupancy of two Pumilio molecules on a single hunchback NRE.

机译:一个驼背NRE上两个Pumilio分子的共同占用。

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摘要

Pumilio controls a number of processes in eukaryotes, including the translational repression of hunchback (hb) mRNA in early Drosophila embryos. The Pumilio Puf domain binds to a pair of 32 nucleotide (nt) Nanos response elements (NRE1 and NRE2) within the 3' untranslated region of hb mRNA. Despite the elucidation of structures of human Pumilio Puf domain in complex with hb RNA elements, the nature of hb mRNA recognition remains unclear. In particular, the site that mediates regulation in vivo is significantly larger than the 8-10-nt RNA elements bound to single Puf molecules in crystal structures. Here we present biophysical and biochemical data that partially resolve the paradox. We show that each NRE is composed of two binding sites (Box A and Box B) and that two Puf domains can co-occupy a single NRE. The Puf domains have a higher affinity for the 3' Box B site than the 5' Box A site; binding to the intact NRE appears to be cooperative (at least in some experiments). We suggest that the 2 Pumilio:1 NRE complex is the functional regulatory unit in vivo.
机译:Pumilio控制着真核生物的许多过程,包括果蝇早期胚胎中驼背(hb)mRNA的翻译抑制。 Pumilio Puf结构域与hb mRNA 3'非翻译区域内的一对32个核苷酸(nt)Nanos反应元件(NRE1和NRE2)结合。尽管阐明了与hb RNA元件复合的人Pumilio Puf结构域的结构,但hb mRNA识别的本质仍不清楚。特别地,在体内介导调节的位点明显大于与晶体结构中单个Puf分子结合的8-10-nt RNA元件。在这里,我们提出了部分解决悖论的生物物理和生化数据。我们显示每个NRE由两个结合位点(框A和框B)组成,并且两个Puf域可以共同占据一个NRE。 Puf域对3'Box B位点的亲和力高于5'Box A位点;与完整的NRE结合似乎是协作的(至少在某些实验中如此)。我们建议2 Pumilio:1 NRE复合物是体内的功能性调节单位。

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