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Postnatal brain and skull growth in an Apert syndrome mouse model

机译:Postnatal脑和颅骨增长在锥体综合征小鼠模型中

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摘要

Craniofacial and neural tissues develop in concert throughout pre- and postnatal growth. FGFR-related craniosynostosis syndromes, such as Apert syndrome (AS), are associated with specific phenotypes involving both the skull and the brain. We analyzed the effects of the FGFR P253R mutation for Apert syndrome using the Fgfr2+/P253R mouse to evaluate the effects of this mutation on these two tissues over the course of development from day of birth (P0) to postnatal day 2 (P2). Three-dimensional magnetic resonance microscopy and computed tomography images were acquired from Fgfr2+/P253R mice and unaffected littermates at P0 (N=28) and P2 (N=23). 3D coordinate data for 23 skull and 15 brain landmarks were statistically compared between groups. Results demonstrate that the Fgfr2+/P253R mice show reduced growth in the facial skeleton and the cerebrum, while the height and width of the neurocranium and caudal regions of the brain show increased growth relative to unaffected littermates. This localized correspondence of differential growth patterns in skull and brain point to their continued interaction through development and suggest that both tissues display divergent postnatal growth patterns relative to unaffected littermates. However, the change in the skull-brain relationship from P0 to P2 implies that each tissue affected by the mutation retains a degree of independence, rather than one tissue directing the development of the other.
机译:颅面和神经组织在整个产前和产后生长过程中都会协调发展。诸如Apert综合征(AS)等与FGFR相关的颅突融合症与涉及颅骨和大脑的特定表型有关。我们使用Fgfr2 + / P253R 小鼠分析了FGFR P253R突变对Apert综合征的影响,以评估该突变对从出生(P0)到出生的整个发育过程中这两种组织的影响。产后第2天(P2)。从Fgfr2 + / P253R 小鼠获取三维磁共振显微镜和计算机断层扫描图像,并在P0(N = 28)和P2(N = 23)的同窝出生。在两组之间统计比较了23个头骨和15个脑标志的3D坐标数据。结果表明,Fgfr2 + / P253R 小鼠的面部骨骼和大脑生长减少,而相对于未受影响的同窝仔,大脑的神经颅骨和尾部区域的高度和宽度均显示增长。头骨和大脑中不同生长方式的这种局部对应关系表明它们通过发育而持续相互作用,这表明相对于未受影响的同窝仔来说,两种组织均显示出不同的出生后生长方式。但是,从P0到P2的颅脑关系的变化意味着受突变影响的每个组织都保持一定程度的独立性,而不是一个组织指导另一个组织的发育。

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