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微弱小球(flb)表型剖析:外胚层早期相互作用对果蝇中枢神经系统发育的决定作用

Dissection of the faint little ball (flb) phenotype: determination of the development of the Drosophila central nervous system by early interactions in the ectoderm.

作者信息

Raz E, Shilo B Z

机构信息

Department of Molecular Genetics and Virology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Development. 1992 Jan;114(1):113-23. doi: 10.1242/dev.114.1.113.

Abstract

The complex embryonic phenotype of mutations in the faint little ball (flb) locus, encoding the Drosophila EGF receptor homolog (DER), was dissected by temperature shifts of a temperature-sensitive allele. We show that the phenotype can be resolved into at least five components, which are temporally and spatially distinct. Most notably, the central nervous system (CNS) phenotype is determined at two separate phases. A severe collapse results from early defects in the DER-expressing ectodermal cells from which neuroblasts and midline glial cells deaminate. We thus suggest that DER activity is crucial for interactions that occur in the ectoderm at an early stage, and determine the fate of neuronal and glial cell lineages. This finding explains how a severe CNS phenotype is generated in flb embryos, in spite of the absence of expression of the protein in neuronal cells. In a second phase, during germ band retraction, the flb function is required specifically in the three pairs of midline glial cells (MG). In the absence of a functional DER protein, these cells die or fail to differentiate correctly, resulting in a fused commissure phenotype.

摘要

编码果蝇表皮生长因子受体同源物(DER)的微弱小球(flb)基因座突变的复杂胚胎表型,通过对一个温度敏感等位基因进行温度转换来剖析。我们表明,该表型可分解为至少五个成分,它们在时间和空间上是不同的。最值得注意的是,中枢神经系统(CNS)表型在两个不同阶段确定。严重的崩溃源于表达DER的外胚层细胞早期缺陷,神经母细胞和中线胶质细胞从中脱氨基。因此,我们认为DER活性对于早期在外胚层发生的相互作用至关重要,并决定神经元和胶质细胞谱系的命运。这一发现解释了尽管flb胚胎中神经元细胞中不存在该蛋白质的表达,但仍如何产生严重的CNS表型。在第二阶段,在胚带收缩期间,flb功能特别在三对中线胶质细胞(MG)中是必需的。在缺乏功能性DER蛋白的情况下,这些细胞死亡或未能正确分化,导致连合融合表型。

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