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Mutations in Caenorhabditis briggsae identify new genes important for limiting the response to EGF signaling during vulval development

机译:轻型秀丽隐杆线虫突变鉴定出新基因,这些新基因对于限制外阴发育过程中对EGF信号传导的反应至关重要

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Studies of vulval development in the nematode C. elegans have identified many genes that are involved in cell division and differentiation processes. Some of these encode components of conserved signal transduction pathways mediated by EGF, Notch, and Wnt. To understand how developmental mechanisms change during evolution, we are doing a comparative analysis of vulva formation in C. briggsae, a species that is closely related to C. elegans. Here, we report 14 mutations in 7 Multivulva (Muv) genes in C. briggsae that inhibit inappropriate division of vulval precursors. We have developed a new efficient and cost-effective gene mapping method to localize Muv mutations to small genetic intervals on chromosomes, thus facilitating cloning and functional studies. We demonstrate the utility of our method by determining molecular identities of three of the Muv genes that include orthologs of Cel-lin-1 (ETS) and Cel-lin-31 (Winged-Helix) of the EGF-Ras pathway and Cel-pry-1 (Axin), of the Wnt pathway. The remaining four genes reside in regions that lack orthologs of known C. elegans Muv genes. Inhibitor studies demonstrate that the Muv phenotype of all four new genes is dependent on the activity of the EGF pathway kinase, MEK. One of these, Cbr-lin(gu167), shows modest increase in the expression of Cbr-lin-3/EGF compared to wild type. These results argue that while Cbr-lin(gu167) may act upstream of Cbr-lin-3/EGF, the other three genes influence the EGF pathway downstream or in parallel to Cbr-lin-3. Overall, our findings demonstrate that the genetic program underlying a conserved developmental process includes both conserved and divergent functional contributions.
机译:线虫秀丽隐杆线虫的外阴发育研究已经鉴定出许多与细胞分裂和分化过程有关的基因。其中一些编码由EGF,Notch和Wnt介导的保守信号转导途径的成分。为了了解进化机制在进化过程中如何变化,我们正在对与秀丽隐杆线虫密切相关的布里格球藻的外阴形成进行比较分析。在这里,我们报告了C. briggsae中7个Multivulva(Muv)基因的14个突变,这些突变抑制了外阴前体的不适当分裂。我们已经开发了一种新的有效且具有成本效益的基因作图方法,以将Muv突变定位在染色体上较小的遗传区间,从而促进克隆和功能研究。我们通过确定三个Muv基因的分子身份来证明我们方法的实用性,这三个基因包括EGF-Ras途径和Cel-pry的Cel-lin-1(ETS)和Cel-lin-31(Winged-Helix)直系同源物-1(Axin),位于Wnt途径。其余四个基因位于缺少已知秀丽隐杆线虫Muv基因直系同源物的区域。抑制剂研究表明,所有四个新基因的Muv表型均取决于EGF途径激酶MEK的活性。其中之一是Cbr-lin(gu167),与野生型相比,Cbr-lin-3 / EGF的表达适度增加。这些结果表明,尽管Cbr-lin(gu167)可能在Cbr-lin-3 / EGF的上游起作用,但其他三个基因会影响Cbr-lin-3下游或与之平行的EGF途径。总体而言,我们的发现表明,保守的发育过程所基于的遗传程序包括保守的和不同的功能性贡献。

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