Mouse Imaging Centre (MICe), Hospital for Sick Children, Toronto, Ontario, Canada.
Autism Res. 2011 Oct;4(5):368-76. doi: 10.1002/aur.215. Epub 2011 Aug 31.
Magnetic resonance imaging (MRI) has been used quite extensively for examining morphological changes in human and animal brains. One of the many advantages to examining mouse models of human autism is that we are able to examine single gene targets, like that of Neuroligin3 R451C knockin (NL3 KI), which has been directly implicated in human autism. The NL3 KI mouse model has marked volume differences in many different structures in the brain: gray matter structures, such as the hippocampus, the striatum, and the thalamus, were all found to be smaller in the NL3 KI. Further, many white matter structures were found to be significantly smaller, such as the cerebral peduncle, corpus callosum, fornix/fimbria, and internal capsule. Fractional anisotropy measurements in these structures were also measured, and no differences were found. The volume changes in the white matter regions, therefore, are not due to a general breakdown in the microstructure of the tissue and seem to be caused by fewer axons or less mature axons. A larger radial diffusivity was also found in localized regions of the corpus callosum and cerebellum. The corpus callosal changes are particularly interesting as the thinning (or reduced volume) of the corpus callosum is a consistent finding in autism. This suggests that the NL3 KI model may be useful for examining white matter changes associated with autism.
磁共振成像(MRI)已被广泛应用于检查人类和动物大脑的形态变化。检查人类自闭症的小鼠模型的众多优势之一是,我们能够检查单一基因靶点,如 Neuroligin3 R451C 敲入(NL3 KI),该靶点直接与人类自闭症有关。NL3 KI 小鼠模型的大脑中有许多不同结构的体积存在明显差异:灰质结构,如海马体、纹状体和丘脑,在 NL3 KI 中均较小。此外,许多白质结构也明显较小,如大脑脚、胼胝体、穹窿/海马伞和内囊。这些结构的各向异性分数测量也进行了测量,但未发现差异。因此,白质区域的体积变化不是由于组织的微观结构普遍破裂造成的,似乎是由于轴突较少或轴突不成熟造成的。在胼胝体和小脑的局部区域还发现了更大的放射状扩散。胼胝体的变化尤其有趣,因为胼胝体变薄(或体积减小)是自闭症的一个一致发现。这表明 NL3 KI 模型可能有助于检查与自闭症相关的白质变化。
