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果蝇胚胎早期背腹模式形成的尺寸依赖性调控。

Size-dependent regulation of dorsal-ventral patterning in the early Drosophila embryo.

机构信息

Division of Biology, California Institute of Technology, Pasadena, CA, USA.

出版信息

Dev Biol. 2013 Sep 1;381(1):286-99. doi: 10.1016/j.ydbio.2013.06.020. Epub 2013 Jun 22.

Abstract

How natural variation in embryo size affects patterning of the Drosophila embryo dorsal-ventral (DV) axis is not known. Here we examined quantitatively the relationship between nuclear distribution of the Dorsal transcription factor, boundary positions for several target genes, and DV axis length. Data were obtained from embryos of a wild-type background as well as from mutant lines inbred to size select embryos of smaller or larger sizes. Our data show that the width of the nuclear Dorsal gradient correlates with DV axis length. In turn, for some genes expressed along the DV axis, the boundary positions correlate closely with nuclear Dorsal levels and with DV axis length; while the expression pattern of others is relatively constant and independent of the width of the Dorsal gradient. In particular, the patterns of snail (sna) and ventral nervous system defective (vnd) correlate with nuclear Dorsal levels and exhibit scaling to DV length; while the pattern of intermediate neuroblasts defective (ind) remains relatively constant with respect to changes in Dorsal and DV length. However, in mutants that exhibit an abnormal expansion of the Dorsal gradient which fails to scale to DV length, only sna follows the Dorsal distribution and exhibits overexpansion; in contrast, vnd and ind do not overexpand suggesting some additional mechanism acts to refine the dorsal boundaries of these two genes. Thus, our results argue against the idea that the Dorsal gradient works as a global system of relative coordinates along the DV axis and suggest that individual targets respond to changes in embryo size in a gene-specific manner.

摘要

胚胎大小的自然变异如何影响果蝇胚胎背腹(DV)轴的模式尚不清楚。在这里,我们定量研究了 Dorsal 转录因子的核分布、几个靶基因的边界位置与 DV 轴长度之间的关系。数据来自野生型背景的胚胎,以及内交至较小或较大大小胚胎的突变系。我们的数据表明,核 Dorsal 梯度的宽度与 DV 轴长度相关。反过来,对于一些在 DV 轴上表达的基因,边界位置与核 Dorsal 水平和 DV 轴长度密切相关;而其他基因的表达模式相对稳定,与 Dorsal 梯度的宽度无关。特别是 snail(sna)和 ventral nervous system defective(vnd)的表达模式与核 Dorsal 水平相关,并与 DV 长度呈比例关系;而 intermediate neuroblasts defective(ind)的表达模式相对于 Dorsal 和 DV 长度的变化保持相对稳定。然而,在那些表现出 Dorsal 梯度异常扩张但不能与 DV 长度成比例缩放的突变体中,只有 sna 遵循 Dorsal 分布并表现出过度扩张;相比之下,vnd 和 ind 并没有过度扩张,这表明存在一些额外的机制来细化这两个基因的背侧边界。因此,我们的结果反对 Dorsal 梯度作为 DV 轴上相对坐标的全局系统的观点,并表明个别靶基因以基因特异性的方式对胚胎大小的变化作出反应。

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