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Identification of compounds that decrease the fidelity of start codon recognition by the eukaryotic translational machinery.

机译:通过真核翻译机器鉴定降低起始密码子识别保真度的化合物。

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Translation initiation in eukaryotes involves more than a dozen protein factors. Alterations in six factors have been found to reduce the fidelity of start codon recognition by the ribosomal preinitiation complex in yeast, a phenotype referred to as Sui(-). No small molecules are known that affect the fidelity of start codon recognition. Such compounds would be useful tools for probing the molecular mechanics of translation initiation and its regulation. To find compounds with this effect, we set up a high-throughput screen using a dual luciferase assay in S. cerevisiae. Screening of over 55,000 compounds revealed two structurally related molecules that decrease the fidelity of start codon selection by approximately twofold in the dual luciferase assay. This effect was confirmed using additional in vivo assays that monitor translation from non-AUG start codons. Both compounds increase translation of a natural upstream open reading frame previously shown to initiate translation at a UUG. The compounds were also found to exacerbate increased use of UUG as a start codon (Sui(-) phenotype) conferred by haploinsufficiency of wild-type eukaryotic initiation factor (eIF) 1, or by mutation in eIF1. Furthermore, the effects of the compounds are suppressed by overexpressing eIF1, which is known to restore the fidelity of start codon selection in strains harboring Sui(-) mutations in various other initiation factors. Together, these data strongly suggest that the compounds affect the translational machinery itself to reduce the accuracy of selecting AUG as the start codon.
机译:真核生物的翻译起始涉及十几种蛋白质因子。已经发现六个因素的改变会降低酵母中核糖体预启动复合物(称为Sui(-)的表型)的起始密码子识别的保真度。没有小分子会影响起始密码子识别的保真度。这样的化合物将是探测翻译起始及其调控的分子力学的有用工具。为了找到具有这种作用的化合物,我们在酿酒酵母中使用双重荧光素酶测定法建立了高通量筛选。超过55,000种化合物的筛选显示出两个结构相关的分子,它们在双荧光素酶测定中将起始密码子选择的保真度降低了约两倍。使用监测非AUG起始密码子翻译的其他体内测定法证实了这种效果。两种化合物均增加了天然上游开放阅读框的翻译,先前显示可在UUG启动翻译。还发现这些化合物加剧了由于野生型真核生物起始因子(eIF)1的单倍不足或eIF1突变而增加的UUG作为起始密码子(Sui(-)表型)的使用。此外,化合物的作用可通过过表达eIF1来抑制,eIF1可以恢复在各种其他起始因子中带有Sui(-)突变的菌株中恢复起始密码子选择的保真度。总之,这些数据强烈表明这些化合物影响翻译机制本身,从而降低了选择AUG作为起始密码子的准确性。

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