首页> 外文期刊>Cellular and Molecular Neurobiology >D-serine and serine racemase are localized to neurons in the adult mouse and human forebrain.
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D-serine and serine racemase are localized to neurons in the adult mouse and human forebrain.

机译:D-丝氨酸和丝氨酸消旋酶位于成年小鼠和人类前脑的神经元中。

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摘要

D-Serine, a co-agonist at the NMDA receptor (NMDAR), is synthesized from L-serine by the enzyme serine racemase (SR), which is heavily expressed in the forebrain. Although SR was originally reported to be localized exclusively to astrocytes, recent conditional knock out results demonstrate that little SR is expressed in forebrain astrocytes. As a consequence, the cellular location of its product, D-serine, in the brain is also uncertain. Immunocytochemistry now indicates that SR is expressed primarily in forebrain glutamatergic neurons with the remainder in GABAergic interneurons. We utilized SR deficient (SR-/-) mice, which have <15 % of normal D-serine levels, to validate and optimize a D-serine immunohistochemical method. Nearly all of the D-serine in neocortex and hippocampus (HP) is found in neurons, with virtually no D-serine co-localizing with two astrocyte markers. Interestingly, only a subset of the D-serine positive neurons contained SR in the neocortex and HP. Greater than half of the D-serine positive neurons were GABAergic interneurons, with a majority of these neurons containing parvalbumin and/or somatostatin. Only ~25-40 % of interneurons expressed SR in the neocortex and HP. Finally, we demonstrate in human post-mortem neocortex that SR is found in both excitatory and inhibitory neurons, but not in S100β-containing astrocytes. In sum, these findings conclusively demonstrate that the majority of D-serine is both synthesized and stored in neurons. It will be important to determine the functional significance for the separation of synthesis and storage of D-serine in neurons, as well as the presence of this NMDAR co-agonist in GABAergic interneurons.
机译:D-Serine是NMDA受体(NMDAR)的辅助激动剂,是通过丝氨酸消旋酶(SR)从L-丝氨酸合成的,该酶在前脑中大量表达。尽管SR最初被报道仅定位于星形胶质细胞,但最近的条件敲除结果表明前脑星形胶质细胞中几乎没有SR表达。结果,其产物D-丝氨酸在脑中的细胞位置也不确定。免疫细胞化学现在表明SR主要在前脑谷氨酸能神经元中表达,其余在GABA能神经元中表达。我们利用SR缺陷(SR-/-)小鼠(其正常D-丝氨酸水平的<15%)来验证和优化D-丝氨酸免疫组化方法。新皮层和海马(HP)中几乎所有D-丝氨酸都存在于神经元中,几乎没有D-丝氨酸与两个星形胶质细胞标记共定位。有趣的是,仅D-丝氨酸阳性神经元的一部分在新皮层和HP中含有SR。 D-丝氨酸阳性神经元的一半以上是GABA能神经元,其中大多数神经元含有小白蛋白和/或生长抑素。只有约25-40%的中间神经元在新皮层和HP中表达SR。最后,我们在人类尸体新皮层中证明,在兴奋性和抑制性神经元中都发现了SR,但在含S100β的星形胶质细胞中却未发现SR。总之,这些发现最终证明了大多数D-丝氨酸都是合成的并存储在神经元中。确定D丝氨酸在神经元中的合成和储存的分离的功能意义,以及这种NMDAR协同激动剂在GABA能性中间神经元中的存在,将非常重要。

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