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揭示大脑皮质兴奋性突触处星形胶质细胞和神经元 GLT-1 共定位的 Na+/K+-ATPase α 同工型的异质性。

Heterogeneity of Astrocytic and Neuronal GLT-1 at Cortical Excitatory Synapses, as Revealed by its Colocalization With Na+/K+-ATPase α Isoforms.

机构信息

Section of Neuroscience and Cell Biology, Department of Experimental and Clinical Medicine, Università Politecnica delle Marche, Ancona, Italy.

Center for Neurobiology of Aging, IRCCS INRCA, Ancona, Italy.

出版信息

Cereb Cortex. 2019 Jul 22;29(8):3331-3350. doi: 10.1093/cercor/bhy203.

DOI:10.1093/cercor/bhy203
PMID:30260367
Abstract

GLT-1, the major glutamate transporter, is expressed at perisynaptic astrocytic processes (PAP) and axon terminals (AxT). GLT-1 is coupled to Na+/K+-ATPase (NKA) α1-3 isoforms, whose subcellular distribution and spatial organization in relationship to GLT-1 are largely unknown. Using several microscopy techniques, we showed that at excitatory synapses α1 and α3 are exclusively neuronal (mainly in dendrites and in some AxT), while α2 is predominantly astrocytic. GLT-1 displayed a differential colocalization with α1-3. GLT-1/α2 and GLT-1/α3 colocalization was higher in GLT-1 positive puncta partially (for GLT-1/α2) or almost totally (for GLT-1/α3) overlapping with VGLUT1 positive terminals than in nonoverlapping ones. GLT-1 colocalized with α2 at PAP, and with α1 and α3 at AxT. GLT-1 and α2 gold particles were ∼1.5-2 times closer than GLT-1/α1 and GLT-1/α3 particles. GLT-1/α2 complexes (edge to edge interdistance of gold particles ≤50 nm) concentrated at the perisynaptic region of PAP membranes, whereas neuronal GLT-1/α1 and GLT-1/α3 complexes were fewer and more uniformly distributed in AxT. These data unveil different composition of GLT-1 and α subunits complexes in the glial and neuronal domains of excitatory synapses. The spatial organization of GLT-1/α1-3 complexes suggests that GLT-1/NKA interaction is more efficient in astrocytes than in neurons, further supporting the dominant role of astrocytic GLT-1 in glutamate homeostasis.

摘要

GLT-1,即主要的谷氨酸转运体,在突触旁星形胶质细胞突起(PAP)和轴突末梢(AxT)表达。GLT-1 与 Na+/K+-ATP 酶(NKA)α1-3 异构体偶联,其亚细胞分布和与 GLT-1 的空间组织在很大程度上尚不清楚。使用几种显微镜技术,我们发现在兴奋性突触上,α1 和 α3 仅存在于神经元中(主要在树突和一些 AxT 中),而 α2 主要存在于星形胶质细胞中。GLT-1 与 α1-3 存在不同的共定位。GLT-1/α2 和 GLT-1/α3 的共定位在与 VGLUT1 阳性末梢部分(对于 GLT-1/α2)或几乎完全(对于 GLT-1/α3)重叠的 GLT-1 阳性斑点中高于不重叠的斑点。GLT-1 在 PAP 处与 α2 共定位,在 AxT 处与 α1 和 α3 共定位。GLT-1 和 α2 金颗粒之间的距离比 GLT-1/α1 和 GLT-1/α3 颗粒之间的距离近 1.5-2 倍。GLT-1/α2 复合物(金颗粒边缘到边缘的间隔距离≤50nm)集中在 PAP 膜的突触旁区域,而神经元 GLT-1/α1 和 GLT-1/α3 复合物较少且在 AxT 中分布更均匀。这些数据揭示了兴奋性突触的胶质和神经元区域中 GLT-1 和 α 亚基复合物的不同组成。GLT-1/α1-3 复合物的空间组织表明,GLT-1/NKA 相互作用在星形胶质细胞中比在神经元中更有效,进一步支持星形胶质细胞 GLT-1 在谷氨酸稳态中的主导作用。

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