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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Characterization of X-linked recessive lethal mutations affecting embryonic morphogenesis in Drosophila melanogaster.
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Characterization of X-linked recessive lethal mutations affecting embryonic morphogenesis in Drosophila melanogaster.

机译:X连锁隐性致死突变影响果蝇果蝇胚胎形态发生的表征。

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摘要

This study attempted to assay the zygotic contribution of X chromosome genes to the genetic control of embryonic morphogenesis in Drosophila melanogaster. A systematic screen for X-linked genes which affect the morphology of the embryo was undertaken, employing the phenotype of whole mount embryos as the major screening criterion. Of 800 EMS-induced lethal mutations analyzed, only 14% were embryonic lethal, and of these only a minority affected embryonic morphogenesis. By recombination and complementation analyses, the mutations that affected embryonic morphogenesis were sequestered into 26 complementation groups. Fourteen of the loci correspond to genes previously identified in a large-scale screen in which fixed cuticles were examined, and 12 new loci have been identified. Most of the mutations which disrupt embryonic morphology had specific and uniform mutant phenotypes. Mutations were recovered which disrupt major morphogenetic events such as gastrulation, germ band retraction and head involution. No mutations were found which arrest the embryos prior to blastoderm formation. However, a novel class was found, one comprised of mutations which interfere with the development of internal structures but not cuticular structures. Nevertheless, saturation of the X chromosome for genes important for embryonic morphogenesis is probably incomplete.
机译:这项研究试图测定X染色体基因对果蝇果蝇胚胎形态发生的遗传控制的合子作用。以整座胚胎表型为主要筛选标准,对影响胚胎形态的X连锁基因进行了系统筛选。在分析的800个EMS诱导的致死突变中,只有14%是胚胎致死的,其中只有少数会影响胚胎的形态发生。通过重组和互补分析,影响胚胎形态发生的突变被隔离为26个互补组。十四个基因座对应于先前在大规模屏幕中鉴定出的基因,该大分子筛查了固定的角质层,并鉴定出了十二个新基因座。大多数破坏胚胎形态的突变具有特定且统一的突变表型。恢复了突变,这些突变破坏了主要的形态发生事件,例如胃形成,胚芽回缩和头向内退化。未发现在胚盘形成之前将胚胎停滞的突变。然而,发现了一种新颖的类别,其中一类包括干扰内部结构而不是表皮结构发育的突变。然而,对于胚胎形态发生重要的基因,X染色体的饱和度可能是不完整的。

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