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发育中小鼠视网膜中质膜和囊泡γ-氨基丁酸转运体的表达

Plasmalemmal and vesicular gamma-aminobutyric acid transporter expression in the developing mouse retina.

作者信息

Guo Chenying, Stella Salvatore L, Hirano Arlene A, Brecha Nicholas C

机构信息

Department of Neurobiology, David Geffen School of Medicine at UCLA, University of California, Los Angeles, California 90095, USA.

出版信息

J Comp Neurol. 2009 Jan 1;512(1):6-26. doi: 10.1002/cne.21846.

Abstract

Plasmalemmal and vesicular gamma-aminobutyric acid (GABA) transporters influence neurotransmission by regulating high-affinity GABA uptake and GABA release into the synaptic cleft and extracellular space. Postnatal expression of the plasmalemmal GABA transporter-1 (GAT-1), GAT-3, and the vesicular GABA/glycine transporter (VGAT) were evaluated in the developing mouse retina by using immunohistochemistry with affinity-purified antibodies. Weak transporter immunoreactivity was observed in the inner retina at postnatal day 0 (P0). GAT-1 immunostaining at P0 and at older ages was in amacrine and displaced amacrine cells in the inner nuclear layer (INL) and ganglion cell layer (GCL), respectively, and in their processes in the inner plexiform layer (IPL). At P10, weak GAT-1 immunostaining was in Müller cell processes. GAT-3 immunostaining at P0 and older ages was in amacrine cells and their processes, as well as in Müller cells and their processes that extended radially across the retina. At P10, Müller cell somata were observed in the middle of the INL. VGAT immunostaining was present at P0 and older ages in amacrine cells in the INL as well as processes in the IPL. At P5, weak VGAT immunostaining was also observed in horizontal cell somata and processes. By P15, the GAT and VGAT immunostaining patterns appear similar to the adult immunostaining patterns; they reached adult levels by about P20. These findings demonstrate that GABA uptake and release are initially established in the inner retina during the first postnatal week and that these systems subsequently mature in the outer retina during the second postnatal week.

摘要

质膜和囊泡γ-氨基丁酸(GABA)转运体通过调节高亲和力GABA摄取以及GABA释放到突触间隙和细胞外空间来影响神经传递。通过使用亲和纯化抗体进行免疫组织化学,在发育中的小鼠视网膜中评估了质膜GABA转运体-1(GAT-1)、GAT-3和囊泡GABA/甘氨酸转运体(VGAT)的出生后表达。在出生后第0天(P0),在内视网膜中观察到较弱的转运体免疫反应性。P0及更大年龄时,GAT-1免疫染色分别在内核层(INL)和神经节细胞层(GCL)的无长突细胞和移位无长突细胞中,以及在内网状层(IPL)的它们的突起中。在P10时,GAT-1免疫染色较弱,存在于穆勒细胞突起中。P0及更大年龄时,GAT-3免疫染色存在于无长突细胞及其突起中,以及穆勒细胞及其径向穿过视网膜的突起中。在P10时,在INL中部观察到穆勒细胞胞体。VGAT免疫染色在P0及更大年龄时存在于INL的无长突细胞以及IPL的突起中。在P5时,在水平细胞胞体和突起中也观察到较弱的VGAT免疫染色。到P15时,GAT和VGAT免疫染色模式与成年免疫染色模式相似;它们在大约P20时达到成年水平。这些发现表明,GABA摄取和释放最初在出生后第一周内在内视网膜中建立,并且这些系统随后在出生后第二周在外视网膜中成熟。

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