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维甲酸描绘了出生后大脑皮质中神经元可塑性的地形图。

Retinoic acid delineates the topography of neuronal plasticity in postnatal cerebral cortex.

作者信息

Wagner Elisabeth, Luo Tuanlian, Sakai Yasuo, Parada Luis F, Dräger Ursula C

机构信息

Eunice Kennedy Shriver Center for Mental Retardation, 200 Trapelo Road., Waltham, MA 02452, USA.

出版信息

Eur J Neurosci. 2006 Jul;24(2):329-40. doi: 10.1111/j.1460-9568.2006.04934.x. Epub 2006 Jul 12.

Abstract

Retinoic acid is well recognized to promote neuronal differentiation in the embryonic nervous system, but how it influences the postnatal cerebral cortex remains largely unknown. The domain of highest retinoic acid actions in the cortex of the mouse constricts postnatally to a narrow band that includes the dorsal visual stream and the attentional and executive networks. This band of cortex, which is distinguished by the retinoic acid-synthesizing enzyme RALDH3, exhibits signs of delayed maturation and enhanced plasticity compared to the surrounding cortex, as indicated by suppression of parvalbumin, neurofilament, cytochrome oxidase and perineuronal net maturation, and persistence of the embryonic, polysialated form of the neural cell-adhesion molecule PSA-NCAM. During the first postnatal week, the RALDH3-expressing territory translocates in the caudal cortex from the medial limbic lobe to the adjacent neocortex. This topographical shift requires the neurotrophin NT-3 because in mice lacking neuronal NT-3 the RALDH3 enzyme maintains its early postnatal pattern up to adulthood. In the NT-3-null mutants, expression of the markers, whose topography colocalizes with RALDH3 in the normal cortex, matches the abnormal RALDH3 pattern. This indicates that the uneven retinoic acid distribution serves a role in patterning the maturation and to some extent function of the normal postnatal cerebral cortex.

摘要

视黄酸在胚胎神经系统中促进神经元分化已得到广泛认可,但它如何影响出生后的大脑皮层在很大程度上仍不清楚。小鼠皮层中视黄酸作用最强的区域在出生后会收缩成一条狭窄的带,包括背侧视觉通路以及注意力和执行网络。这条皮层带以视黄酸合成酶RALDH3为特征,与周围皮层相比,显示出成熟延迟和可塑性增强的迹象,这表现为小白蛋白、神经丝、细胞色素氧化酶和神经元周围网络成熟受到抑制,以及神经细胞黏附分子PSA-NCAM的胚胎多唾液酸化形式持续存在。在出生后的第一周,表达RALDH3的区域在尾侧皮层中从内侧边缘叶转移到相邻的新皮层。这种地形学上的转变需要神经营养因子NT-3,因为在缺乏神经元NT-3的小鼠中,RALDH3酶在成年前一直保持其出生后的早期模式。在NT-3基因敲除突变体中,那些在正常皮层中地形学上与RALDH3共定位的标记物的表达,与异常的RALDH3模式相匹配。这表明视黄酸分布不均在正常出生后大脑皮层的成熟模式形成以及一定程度的功能方面发挥作用。

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