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首页> 外文期刊>BMC Genomics >Quadruplex DNA in long terminal repeats in maize LTR retrotransposons inhibits the expression of a reporter gene in yeast
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Quadruplex DNA in long terminal repeats in maize LTR retrotransposons inhibits the expression of a reporter gene in yeast

机译:玉米LTR逆转座子长末端重复序列中的四链体DNA抑制酵母中报道基因的表达

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Many studies have shown that guanine-rich DNA sequences form quadruplex structures (G4) in vitro but there is scarce evidence of guanine quadruplexes in vivo. The majority of potential quadruplex-forming sequences (PQS) are located in transposable elements (TEs), especially close to promoters within long terminal repeats of plant LTR retrotransposons. In order to test the potential effect of G4s on retrotransposon expression, we cloned the long terminal repeats of selected maize LTR retrotransposons upstream of the lacZ reporter gene and measured its transcription and translation in yeast. We found that G4s had an inhibitory effect on translation in vivo since “mutants” (where guanines were replaced by adenines in PQS) showed higher expression levels than wild-types. In parallel, we confirmed by circular dichroism measurements that the selected sequences can indeed adopt G4 conformation in vitro. Analysis of RNA-Seq of polyA RNA in maize seedlings grown in the presence of a G4-stabilizing ligand (NMM) showed both inhibitory as well as stimulatory effects on the transcription of LTR retrotransposons. Our results demonstrate that quadruplex DNA located within long terminal repeats of LTR retrotransposons can be formed in vivo and that it plays a regulatory role in the LTR retrotransposon life-cycle, thus also affecting genome dynamics.
机译:许多研究表明,富含鸟嘌呤的DNA序列在体外形成四链体结构(G4),但是在体内几乎没有鸟嘌呤四链体的证据。大多数潜在的四链体形成序列(PQS)位于转座因子(TEs)中,尤其靠近植物LTR逆转座子长末端重复序列内的启动子。为了测试G4对逆转录转座子表达的潜在影响,我们在lacZ报告基因上游克隆了所选玉米LTR逆转座子的长末端重复序列,并测量了其在酵母中的转录和翻译。我们发现G4s在体内对翻译具有抑制作用,因为“突变体”(在PQS中鸟嘌呤被腺嘌呤替代)显示出比野生型更高的表达水平。同时,我们通过圆二色性测量证实了所选的序列确实可以在体外采用G4构象。在G4稳定配体(NMM)存在下生长的玉米幼苗中polyA RNA的RNA-Seq分析显示,对LTR逆转座子的转录既有抑制作用,也有刺激作用。我们的结果表明,位于LTR逆转座子长末端重复序列内的四链体DNA可以在体内形成,并且在LTR逆转座子的生命周期中起调节作用,因此也影响基因组动力学。

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