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A novel small molecule that disrupts a key event during the oocyte-to-embryo transition in C. elegans

机译:一种新型小分子,可在秀丽隐杆线虫卵母细胞向胚胎过渡期间破坏关键事件

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The complex cellular events that occur in response to fertilization are essential for mediating the oocyte-to-embryo transition. Here, we describe a comprehensive small-molecule screen focused on identifying compounds that affect early embryonic events in Caenorhabditis elegans. We identify a single novel compound that disrupts early embryogenesis with remarkable stage and species specificity. The compound, named C22, primarily impairs eggshell integrity, leading to osmotic sensitivity and embryonic lethality. The C22-induced phenotype is dependent upon the upregulation of the LET-607/CREBH transcription factor and its candidate target genes, which primarily encode factors involved in diverse aspects of protein trafficking. Together, our data suggest that in the presence of C22, one or more key components of the eggshell are inappropriately processed, leading to permeable, inviable embryos. The remarkable specificity and reversibility of this compound will facilitate further investigation into the role and regulation of protein trafficking in the early embryo, as well as serve as a tool for manipulating the life cycle for other studies such as those involving aging.
机译:响应受精而发生的复杂细胞事件对于介导卵母细胞向胚胎的转化至关重要。在这里,我们描述了一个全面的小分子筛选,重点是鉴定影响秀丽隐杆线虫早期胚胎事件的化合物。我们确定了一个单一的新型化合物,以显着的阶段和物种特异性破坏了早期的胚胎发生。该化合物名为C22,主要损害蛋壳的完整性,导致渗透敏感性和胚胎致死性。 C22诱导的表型取决于LET-607 / CREBH转录因子及其候选靶基因的上调,后者主要编码参与蛋白质运输各个方面的因子。总之,我们的数据表明,在存在C22的情况下,蛋壳的一种或多种关键成分加工不当,从而导致可渗透的,无法繁殖的胚胎。该化合物的显着特异性和可逆性将促进对早期胚胎中蛋白质运输的作用和调控的进一步研究,并且可作为操纵生命周期的工具,用于其他研究(如涉及衰老的研究)。

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