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Frizzled 1 and frizzled 2 genes function in palate, ventricular septum and neural tube closure: general implications for tissue fusion processes.

机译:卷曲的1和卷曲的2基因在上,、心室间隔和神经管闭合中起作用:对组织融合过程的一般影响。

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摘要

The closure of an open anatomical structure by the directed growth and fusion of two tissue masses is a recurrent theme in mammalian embryology, and this process plays an integral role in the development of the palate, ventricular septum, neural tube, urethra, diaphragm and eye. In mice, targeted mutations of the genes encoding frizzled 1 (Fz1) and frizzled 2 (Fz2) show that these highly homologous integral membrane receptors play an essential and partially redundant role in closure of the palate and ventricular septum, and in the correct positioning of the cardiac outflow tract. When combined with a mutant allele of the planar cell polarity gene Vangl2 (Vangl2(Lp)), Fz1 and/or Fz2 mutations also cause defects in neural tube closure and misorientation of inner ear sensory hair cells. These observations indicate that frizzled signaling is involved in diverse tissue closure processes, defects in which account for some of the most common congenital anomalies in humans.
机译:通过两个组织块的定向生长和融合来闭合开放的解剖结构是哺乳动物胚胎学中的一个经常出现的主题,该过程在in,心室间隔,神经管,尿道、,肌和眼的发育中起着不可或缺的作用。 。在小鼠中,编码卷曲的1(Fz1)和卷曲的2(Fz2)的基因的定向突变表明,这些高度同源的整合膜受体在上late和心室间隔的闭合以及正确定位中起着必不可少且部分重复的作用。心脏流出道。当与平面细胞极性基因Vangl2(Vangl2(Lp))的突变等位基因结合时,Fz1和/或Fz2突变也会引起神经管闭合和内耳感觉毛细胞方向错误的缺陷。这些观察结果表明,卷曲信号传导参与了多种组织闭合过程,这些缺陷是人类最常见的先天性异常的原因。

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