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产前表达 D-天冬氨酸氧化酶导致早期大脑 D-天冬氨酸耗竭,并影响成年后的大脑形态和认知功能。

Prenatal expression of D-aspartate oxidase causes early cerebral D-aspartate depletion and influences brain morphology and cognitive functions at adulthood.

机构信息

CEINGE Biotecnologie Avanzate, 80145, Naples, Italy.

Department of Experimental Medicine, Sapienza University of Rome, 00185, Rome, Italy.

出版信息

Amino Acids. 2020 Apr;52(4):597-617. doi: 10.1007/s00726-020-02839-y. Epub 2020 Mar 17.

DOI:10.1007/s00726-020-02839-y
PMID:32185508
Abstract

The free D-amino acid, D-aspartate, is abundant in the embryonic brain but significantly decreases after birth. Besides its intracellular occurrence, D-aspartate is also present at extracellular level and acts as an endogenous agonist for NMDA and mGlu5 receptors. These findings suggest that D-aspartate is a candidate signaling molecule involved in neural development, influencing brain morphology and behaviors at adulthood. To address this issue, we generated a knockin mouse model in which the enzyme regulating D-aspartate catabolism, D-aspartate oxidase (DDO), is expressed starting from the zygotic stage, to enable the removal of D-aspartate in prenatal and postnatal life. In line with our strategy, we found a severe depletion of cerebral D-aspartate levels (up to 95%), since the early stages of mouse prenatal life. Despite the loss of D-aspartate content, Ddo knockin mice are viable, fertile, and show normal gross brain morphology at adulthood. Interestingly, early D-aspartate depletion is associated with a selective increase in the number of parvalbumin-positive interneurons in the prefrontal cortex and also with improved memory performance in Ddo knockin mice. In conclusion, the present data indicate for the first time a biological significance of precocious D-aspartate in regulating mouse brain formation and function at adulthood.

摘要

游离态 D- 氨基酸,即 D- 天冬氨酸,在胚胎大脑中含量丰富,但在出生后显著减少。除了在细胞内存在,D- 天冬氨酸也存在于细胞外,并作为 NMDA 和 mGlu5 受体的内源性激动剂发挥作用。这些发现表明,D- 天冬氨酸是一种参与神经发育的候选信号分子,影响成年期的大脑形态和行为。为了解决这个问题,我们生成了一种 knockin 小鼠模型,其中调节 D- 天冬氨酸分解代谢的酶,D- 天冬氨酸氧化酶(DDO),从胚胎阶段开始表达,以在产前和产后去除 D- 天冬氨酸。与我们的策略一致,我们发现大脑中 D- 天冬氨酸水平严重耗竭(高达 95%),从小鼠产前生命的早期阶段开始。尽管 D- 天冬氨酸含量丧失,Ddo knockin 小鼠仍具有活力、可育,并在成年期表现出正常的大脑大体形态。有趣的是,早期 D- 天冬氨酸耗竭与前额叶皮层中 parvalbumin 阳性中间神经元数量的选择性增加有关,并且 Ddo knockin 小鼠的记忆表现也得到改善。总之,这些数据首次表明,早期 D- 天冬氨酸在调节成年期小鼠大脑形成和功能方面具有生物学意义。

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