Department of Biological Sciences, University of Alberta, Edmonton, Alberta, Canada.
Dev Dyn. 2011 Feb;240(2):372-83. doi: 10.1002/dvdy.22547.
The loss of Cecr2, which encodes a chromatin remodeling protein, has been associated with the neural tube defect (NTD) exencephaly and open eyelids in mice. Here, we show that two independent mutations of Cecr2 are also associated with specific inner ear defects. Homozygous mutant 18.5 days post coitus (dpc) fetuses exhibited smaller cochleae as well as rotational defects of sensory cells and extra cell rows in the inner ear reminiscent of planar cell polarity (PCP) mutants. Cecr2 was expressed in the neuroepithelium, head mesenchyme, and the cochlear floor. Although limited genetic interaction for NTDs was seen with Vangl2, a microarray analysis of PCP genes did not reveal a direct connection to this pathway. The mechanism of Cecr2 action in neurogenesis and inner ear development is likely complex.
编码染色质重塑蛋白的 Cecr2 缺失与神经管缺陷(NTD)无脑畸形和小鼠睁眼相关。在这里,我们表明 Cecr2 的两个独立突变也与特定的内耳缺陷有关。同源突变的 18.5 天合子(dpc)胎鼠耳蜗较小,感觉细胞和内耳额外细胞列的旋转缺陷类似于平面细胞极性(PCP)突变体。Cecr2 在神经上皮、头部间充质和耳蜗底板中表达。尽管与 Vangl2 观察到 NTDs 的有限遗传相互作用,但 PCP 基因的微阵列分析并未显示与该途径的直接联系。Cecr2 在神经发生和内耳发育中的作用机制可能很复杂。
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