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反向遗传学筛选揭示了斑马鱼中 morpholino 诱导表型和突变体表型之间的相关性较差。

Reverse genetic screening reveals poor correlation between morpholino-induced and mutant phenotypes in zebrafish.

机构信息

Program in Gene Function and Expression, University of Massachusetts Medical School, Worcester, MA 01605, USA.

Hubrecht Institute - KNAW & UMC Utrecht, 3584CT Utrecht, Netherlands.

出版信息

Dev Cell. 2015 Jan 12;32(1):97-108. doi: 10.1016/j.devcel.2014.11.018. Epub 2014 Dec 18.

Abstract

The widespread availability of programmable site-specific nucleases now enables targeted gene disruption in the zebrafish. In this study, we applied site-specific nucleases to generate zebrafish lines bearing individual mutations in more than 20 genes. We found that mutations in only a small proportion of genes caused defects in embryogenesis. Moreover, mutants for ten different genes failed to recapitulate published Morpholino-induced phenotypes (morphants). The absence of phenotypes in mutant embryos was not likely due to maternal effects or failure to eliminate gene function. Consistently, a comparison of published morphant defects with the Sanger Zebrafish Mutation Project revealed that approximately 80% of morphant phenotypes were not observed in mutant embryos, similar to our mutant collection. Based on these results, we suggest that mutant phenotypes become the standard metric to define gene function in zebrafish, after which Morpholinos that recapitulate respective phenotypes could be reliably applied for ancillary analyses.

摘要

如今,可编程的位点特异性核酸酶已经广泛普及,使得在斑马鱼中进行靶向基因敲除成为可能。在这项研究中,我们应用位点特异性核酸酶在 20 多个基因中产生了单个突变的斑马鱼品系。我们发现,只有一小部分基因的突变会导致胚胎发生缺陷。此外,十个不同基因的突变体未能重现已发表的 Morpholino 诱导表型(morphants)。突变体胚胎中不存在表型的情况不太可能是由于母体效应或未能消除基因功能所致。一致地,将已发表的 Morpholino 表型缺陷与 Sanger 斑马鱼突变项目进行比较表明,突变体胚胎中大约 80%的表型缺陷没有被观察到,与我们的突变体集合相似。基于这些结果,我们建议突变表型成为定义斑马鱼中基因功能的标准指标,之后可以可靠地应用重现相应表型的 Morpholinos 进行辅助分析。

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