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Activity of D-amino acid oxidase is widespread in the human central nervous system

机译:D-氨基酸氧化酶的活性在人类中枢神经系统中广泛分布

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摘要

It has been proposed that D-amino acid oxidase (DAO) plays an essential role in degrading D-serine, an endogenous coagonist of N-methyl-D-aspartate (NMDA) glutamate receptors. DAO shows genetic association with amyotrophic lateral sclerosis (ALS) and schizophrenia, in whose pathophysiology aberrant metabolism of D-serine is implicated. Although the pathology of both essentially involves the forebrain, in rodents, enzymatic activity of DAO is hindbrain-shifted and absent in the region. Here, we show activity-based distribution of DAO in the central nervous system (CNS) of humans compared with that of mice. DAO activity in humans was generally higher than that in mice. In the human forebrain, DAO activity was distributed in the subcortical white matter and the posterior limb of internal capsule, while it was almost undetectable in those areas in mice. In the lower brain centers, DAO activity was detected in the gray and white matters in a coordinated fashion in both humans and mice. In humans, DAO activity was prominent along the corticospinal tract, rubrospinal tract, nigrostriatal system, ponto-/olivo-cerebellar fibers, and in the anterolateral system. In contrast, in mice, the reticulospinal tract and ponto-/olivo-cerebellar fibers were the major pathways showing strong DAO activity. In the human corticospinal tract, activity-based staining of DAO did not merge with a motoneuronal marker, but colocalized mostly with excitatory amino acid transporter 2 and in part with GFAP, suggesting that DAO activity-positive cells are astrocytes seen mainly in the motor pathway. These findings establish the distribution of DAO activity in cerebral white matter and the motor system in humans, providing evidence to support the involvement of DAO in schizophrenia and ALS. Our results raise further questions about the regulation of D-serine in DAO-rich regions as well as the physiological/pathological roles of DAO in white matter astrocytes.
机译:已经提出,D-氨基酸氧化酶(DAO)在降解D-丝氨酸中起重要作用,D-丝氨酸是N-甲基-D-天冬氨酸(NMDA)谷氨酸受体的内源性激动剂。 DAO显示出与肌萎缩性侧索硬化症(ALS)和精神分裂症的遗传相关,其中涉及D-丝氨酸的异常代谢。尽管两者的病理本质上都涉及前脑,但在啮齿动物中,该区域的DAO的酶促活性发生了后脑移位和缺失。在这里,我们显示了与小鼠相比,DAO在人的中枢神经系统(CNS)中基于活动的分布。人的DAO活性通常高于小鼠。在人类前脑中,DAO活性分布在皮质下白质和内囊后肢中,而在小鼠的这些区域中几乎无法检测到。在大脑下部的中部,人和小鼠均以协调的方式在灰色和白色物质中检测到DAO活性。在人类中,DAO活性沿皮质脊髓束,迷路脊髓束,黑质纹状体系统,舟桥/小脑小脑纤维以及前外侧系统突出。相反,在小鼠中,网状脊髓束和桥脑/脂小脑纤维是显示出强大的DAO活性的主要途径。在人的皮质脊髓束中,DAO的基于活性的染色并未与动脑神经标记物融合,而是主要与兴奋性氨基酸转运蛋白2共同定位,部分与GFAP共定位,这表明DAO活性阳性细胞是星形胶质细胞,主要存在于运动途径中。这些发现确定了DAO在人脑白质和运动系统中的分布,为支持DAO参与精神分裂症和ALS提供了证据。我们的结果对DAO丰富区域中D-丝氨酸的调节以及DAO在白质星形胶质细胞中的生理/病理作用提出了进一步的问题。

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