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Notch基因座与果蝇早期神经发生过程中涉及的遗传调控网络。

The Notch locus and the genetic circuitry involved in early Drosophila neurogenesis.

作者信息

Xu T, Rebay I, Fleming R J, Scottgale T N, Artavanis-Tsakonas S

机构信息

Department of Biology, Yale University, New Haven, Connecticut 06511.

出版信息

Genes Dev. 1990 Mar;4(3):464-75. doi: 10.1101/gad.4.3.464.

Abstract

The genetic and molecular analysis of the Notch locus, which codes for a transmembrane protein sharing homology with the mammalian epidermal growth factor, suggests that the Notch protein is involved in a cell interaction mechanism essential for the differentiation of the embryonic nervous system of Drosophila. Taking advantage of the negative complementation between two Notch mutations that affect the extracellular domain of the protein, we have tried to dissect the genetic circuitry in which Notch is integrated by searching for genes whose products may interact with the Notch protein. This genetic screen has led to the identification of a surprisingly restricted set of interacting loci, including Delta and mastermind. Like Notch, both of these genes belong to a group of loci, the neurogenic loci, which have been previously identified by virtue of their similar mutant phenotype affecting early neurogenesis. We extend these studies by systematically exploring interactions between specific mutations in the Notch molecule and the other neurogenic genes. Furthermore, we show that the molecular lesions of two Notch alleles (nd and nd2), which interact dramatically with mastermind mutations, as well as with a mutation affecting the transducin homologous product of the neurogenic locus Enhancer of split, involve changes in the intracellular domain of the protein.

摘要

Notch基因座编码一种与哺乳动物表皮生长因子具有同源性的跨膜蛋白,对其进行的遗传和分子分析表明,Notch蛋白参与了果蝇胚胎神经系统分化所必需的细胞相互作用机制。利用影响该蛋白胞外结构域的两个Notch突变之间的负互补作用,我们试图通过寻找其产物可能与Notch蛋白相互作用的基因,来剖析Notch所整合的遗传回路。这种遗传筛选已导致鉴定出一组令人惊讶的有限的相互作用基因座,包括Delta和mastermind。与Notch一样,这两个基因都属于一组基因座,即神经源基因座,它们先前已因其影响早期神经发生的相似突变表型而被鉴定出来。我们通过系统地探索Notch分子中的特定突变与其他神经源基因之间的相互作用来扩展这些研究。此外,我们表明,两个Notch等位基因(nd和nd2)的分子损伤,它们与mastermind突变以及影响神经源基因座分裂增强子的转导素同源产物的突变发生显著相互作用,涉及该蛋白胞内结构域的变化。

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