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基因表达和星形胶质细胞过程的发育调控可能解释了海马体的选择性脆弱性。

Developmental regulation of gene expression and astrocytic processes may explain selective hippocampal vulnerability.

机构信息

Department of Psychiatry and Behavioral Sciences, UC Davis, Sacramento, California 95817, USA.

出版信息

Hippocampus. 2011 Feb;21(2):142-9. doi: 10.1002/hipo.20730.

Abstract

The hippocampus plays a central role in the brain network that is essential for memory function. Paradoxically, the hippocampus is also the brain structure that is most sensitive to hypoxic-ischemic episodes. Here, we show that the expression of genes associated with glycolysis and glutamate metabolism in astrocytes and the coverage of excitatory synapses by astrocytic processes undergo significant decreases in the CA1 field of the monkey hippocampus during postnatal development. Given the established role of astrocytes in the regulation of glutamate concentration in the synaptic cleft, our findings suggest that a developmental decrease in astrocytic processes could underlie the selective vulnerability of CA1 during hypoxic-ischemic episodes in adulthood, its decreased susceptibility to febrile seizures with age, as well as contribute to the emergence of selective, adultlike memory function.

摘要

海马体在大脑网络中起着核心作用,大脑网络对记忆功能至关重要。矛盾的是,海马体也是对缺氧缺血发作最敏感的大脑结构。在这里,我们发现,在猴子海马体的 CA1 区,在出生后的发育过程中,与糖酵解和谷氨酸代谢相关的基因在星形胶质细胞中的表达以及兴奋性突触被星形胶质细胞过程覆盖的情况显著减少。鉴于星形胶质细胞在调节突触间隙中谷氨酸浓度方面的既定作用,我们的研究结果表明,星形胶质细胞过程的发育性减少可能是 CA1 在成年缺氧缺血发作中选择性易损性的基础,其随着年龄的增长对发热性癫痫的敏感性降低,以及有助于出现选择性的、成人样的记忆功能。

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