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腹侧胰腺的器官发生需要六同源框基因依赖性组织定位。

Hex homeobox gene-dependent tissue positioning is required for organogenesis of the ventral pancreas.

作者信息

Bort Roque, Martinez-Barbera Juan Pedro, Beddington Rosa S P, Zaret Kenneth S

机构信息

Cell and Developmental Biology Program, Fox Chase Cancer Center, 7701 Burholme Aveue, Philadelphia, PA 19111, USA.

出版信息

Development. 2004 Feb;131(4):797-806. doi: 10.1242/dev.00965. Epub 2004 Jan 21.

DOI:10.1242/dev.00965
PMID:14736744
Abstract

In animal development, digestive tissues emerge from different positions of the endoderm as a result of patterning signals from overlying mesoderm. Although embryonic tissue movement during gastrulation generates an initial positional relationship between the endoderm and mesoderm, the role of subsequent endoderm movement against the mesoderm in patterning is unknown. At embryonic day 8.5 in the mouse, proliferation of cells at the leading edge of ventral-lateral endoderm, where the liver and ventral pancreas emerge, helps close off the foregut. During this time, the endoderm grows adjacent to and beyond the cardiogenic mesoderm, an inducer of the liver program and an inhibitor of the pancreas program. The homeobox gene Hex is expressed in this endoderm cell domain and in the liver and ventral pancreas buds, after organogenesis. We have found that in Hex(-/-) embryos, there is a complete failure in ventral pancreatic specification, while the liver program is still induced. However, when Hex-null ventral endoderm is isolated prior to its interaction with cardiogenic mesoderm and is cultured in vitro, it activates early pancreas genes. We found that Hex controls the proliferation rate, and thus the positioning, of the leading edge of endoderm cells that grow beyond the cardiogenic mesoderm, during gut tube closure. Thus, Hex-controlled positioning of endoderm cells beyond cardiogenic mesoderm dictates ventral pancreas specification. Other endodermal transcription factors may also function morphogenetically rather than by directly regulating tissue-specific programs.

摘要

在动物发育过程中,由于来自上覆中胚层的模式信号,消化组织从内胚层的不同位置产生。尽管原肠胚形成期间的胚胎组织运动在内胚层和中胚层之间产生了初始位置关系,但随后内胚层相对于中胚层的运动在模式形成中的作用尚不清楚。在小鼠胚胎第8.5天,肝和腹侧胰腺出现的腹侧外侧内胚层前缘的细胞增殖有助于关闭前肠。在此期间,内胚层生长至与心脏中胚层相邻并延伸超过心脏中胚层,心脏中胚层是肝脏程序的诱导物和胰腺程序的抑制剂。同源框基因Hex在这个内胚层细胞区域以及器官发生后的肝脏和腹侧胰腺芽中表达。我们发现,在Hex基因敲除(Hex-/-)胚胎中,腹侧胰腺特化完全失败,而肝脏程序仍被诱导。然而,当在Hex基因缺失的腹侧内胚层与心脏中胚层相互作用之前将其分离并进行体外培养时,它会激活早期胰腺基因。我们发现,Hex在肠管闭合期间控制生长超过心脏中胚层的内胚层细胞前缘的增殖速率,从而控制其定位。因此,Hex控制的内胚层细胞在心脏中胚层之外的定位决定了腹侧胰腺的特化。其他内胚层转录因子也可能在形态发生上发挥作用,而不是直接调节组织特异性程序。

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Development. 2004 Feb;131(4):797-806. doi: 10.1242/dev.00965. Epub 2004 Jan 21.
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