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哺乳动物多梳基因家族成员rae28对后脑和咽弓中Hoxb3表达的调控

Regulation of Hoxb3 expression in the hindbrain and pharyngeal arches by rae28, a member of the mammalian Polycomb group of genes.

作者信息

Tomotsune D, Shirai M, Takihara Y, Shimada K

机构信息

Department of Medical Genetics, Research Institute for Microbial Diseases, Osaka University, 3-1 Yamadaoka, Suita, 565-0871, Osaka, Japan.

出版信息

Mech Dev. 2000 Nov;98(1-2):165-9. doi: 10.1016/s0925-4773(00)00457-3.

Abstract

During animal development, Hox genes are expressed in characteristic, spatially restricted patterns and specify regional identities along the anterior-posterior (A-P) axis. Polycomb group (PcG) proteins in Drosophila repress Hox expression and maintain the expression patterns during development. Mice deficient for homologues of the Drosophila PcG genes, such as M33, bmi1, mel18, rae28 and eed, show altered Hox expression patterns. In this study, we examined the time course of Hoxb3 expression during late gastrulation and early segmentation of rae28-deficient mice. Hoxb3 was expressed ectopically in pharyngeal arch and hindbrain from embryonic day (E) 9.5 and 10.5, respectively. The anterior boundary of ectopic expression in the hindbrain extended gradually in the rostral direction as development proceeded from E10.5 to E12.5. Expression of kreisler and Krox20, which function as positive regulators of Hoxb3 expression, was not affected in rae28-deficient embryos. Analysis of a neural crest marker, p75, in rae28-deficient mice revealed that the neural crest cells begin to ectopically express Hoxb3 after leaving the hindbrain. Our results suggest that rae28 is not required for the establishment but maintenance of Hoxb3 expression.

摘要

在动物发育过程中,Hox基因以特征性的、空间受限的模式表达,并沿前后轴确定区域特征。果蝇中的多梳蛋白组(PcG)蛋白抑制Hox表达,并在发育过程中维持表达模式。缺乏果蝇PcG基因同源物(如M33、bmi1、mel18、rae28和eed)的小鼠表现出Hox表达模式的改变。在本研究中,我们检测了rae28基因缺陷小鼠原肠胚晚期和早期体节形成过程中Hoxb3表达的时间进程。Hoxb3分别在胚胎第(E)9.5天和10.5天在咽弓和后脑异位表达。随着发育从E10.5进展到E12.5,后脑异位表达的前边界逐渐向头侧方向延伸。作为Hoxb3表达正调控因子的kreisler和Krox20的表达在rae28基因缺陷胚胎中不受影响。对rae28基因缺陷小鼠的神经嵴标记物p75的分析表明,神经嵴细胞在离开后脑后开始异位表达Hoxb3。我们的结果表明,rae28对于Hoxb3表达的建立不是必需的,但对于其维持是必需的。

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