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利用合成的 RNAi 抗性转基因在果蝇中验证 RNAi 表型。

Validating RNAi phenotypes in Drosophila using a synthetic RNAi-resistant transgene.

机构信息

Institute of Integrative Biology, University of Liverpool, Liverpool, Merseyside, United Kingdom.

出版信息

PLoS One. 2013 Aug 8;8(8):e70489. doi: 10.1371/journal.pone.0070489. eCollection 2013.

Abstract

RNA interference (RNAi) is a powerful and widely used approach to investigate gene function, but a major limitation of the approach is the high incidence of non-specific phenotypes that arise due to off-target effects. We previously showed that RNAi-mediated knock-down of pico, which encodes the only member of the MRL family of adapter proteins in Drosophila, resulted in reduction in cell number and size leading to reduced tissue growth. In contrast, a recent study reported that pico knockdown leads to tissue dysmorphology, pointing to an indirect role for pico in the control of wing size. To understand the cause of this disparity we have utilised a synthetic RNAi-resistant transgene, which bears minimal sequence homology to the predicted dsRNA but encodes wild type Pico protein, to reanalyse the RNAi lines used in the two studies. We find that the RNAi lines from different sources exhibit different effects, with one set of lines uniquely resulting in a tissue dysmorphology phenotype when expressed in the developing wing. Importantly, the loss of tissue morphology fails to be complemented by co-overexpression of RNAi-resistant pico suggesting that this phenotype is the result of an off-target effect. This highlights the importance of careful validation of RNAi-induced phenotypes, and shows the potential of synthetic transgenes for their experimental validation.

摘要

RNA 干扰 (RNAi) 是一种强大且广泛使用的研究基因功能的方法,但该方法的一个主要限制是由于脱靶效应而产生的非特异性表型的高发生率。我们之前曾表明,RNAi 介导的 pico 敲低,该基因编码果蝇中唯一的 MRL 家族衔接蛋白成员,导致细胞数量和大小减少,从而导致组织生长减少。相比之下,最近的一项研究报告称 pico 敲低导致组织畸形,表明 pico 在控制翅膀大小方面具有间接作用。为了了解这种差异的原因,我们利用了一种合成的 RNAi 抗性转基因,该转基因与预测的 dsRNA 具有最小的序列同源性,但编码野生型 Pico 蛋白,重新分析了这两项研究中使用的 RNAi 系。我们发现,来自不同来源的 RNAi 系表现出不同的效果,一组系在发育中的翅膀中表达时,唯一导致组织畸形表型。重要的是,组织形态的缺失不能通过共表达 RNAi 抗性 pico 来弥补,这表明这种表型是脱靶效应的结果。这凸显了仔细验证 RNAi 诱导的表型的重要性,并展示了合成转基因在实验验证中的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06d3/3738578/fd162f4a70ac/pone.0070489.g001.jpg

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