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rho1亚基的缺失消除了GABA(C)受体的表达,并改变了小鼠视网膜中的视觉处理过程。

Elimination of the rho1 subunit abolishes GABA(C) receptor expression and alters visual processing in the mouse retina.

作者信息

McCall Maureen A, Lukasiewicz Peter D, Gregg Ronald G, Peachey Neal S

机构信息

Department of Psychological and Brain Sciences, University of Louisville, Louisville, Kentucky 40292, USA.

出版信息

J Neurosci. 2002 May 15;22(10):4163-74. doi: 10.1523/JNEUROSCI.22-10-04163.2002.

Abstract

Inhibition is crucial for normal function in the nervous system. In the CNS, inhibition is mediated primarily by the amino acid GABA via activation of two ionotropic GABA receptors, GABA(A) and GABA(C). GABA(A) receptor composition and function have been well characterized, whereas much less is known about native GABA(C) receptors. Differences in molecular composition, anatomical distributions, and physiological properties strongly suggest that GABA(A) receptors and GABA(C) receptors have distinct functional roles in the CNS. To determine the functional role of GABA(C) receptors, we eliminated their expression in mice using a knock-out strategy. Although native rodent GABA(C) receptors are composed of rho1 and rho2 subunits, we show that after rho1 subunit expression was selectively eliminated there was no GABA(C) receptor expression. We assessed GABA(C) receptor function in the retina because GABA(C) receptors are highly expressed on the axon terminals of rod bipolar cells and because this site modulates the visual signal to amacrine and ganglion cells. In GABA(C)rho1 null mice, GABA-evoked responses, normally mediated by GABA(C) receptors, were eliminated, and signaling from rod bipolar cells to third order cells was altered. These data demonstrate that elimination of the GABA(C)rho1 subunit, via gene targeting, results in the absence of GABA(C) receptors in the retina and selective alterations in normal visual processing.

摘要

抑制作用对于神经系统的正常功能至关重要。在中枢神经系统中,抑制作用主要由氨基酸γ-氨基丁酸(GABA)通过激活两种离子型GABA受体——GABA(A)和GABA(C)来介导。GABA(A)受体的组成和功能已得到充分表征,而对于天然的GABA(C)受体却知之甚少。分子组成、解剖分布和生理特性上的差异强烈表明,GABA(A)受体和GABA(C)受体在中枢神经系统中具有不同的功能作用。为了确定GABA(C)受体的功能作用,我们采用基因敲除策略在小鼠中消除了它们的表达。尽管天然啮齿动物的GABA(C)受体由rho1和rho2亚基组成,但我们发现,在选择性消除rho1亚基表达后,没有GABA(C)受体表达。我们在视网膜中评估了GABA(C)受体的功能,因为GABA(C)受体在视杆双极细胞的轴突末端高度表达,并且因为这个部位调节向无长突细胞和神经节细胞传递的视觉信号。在GABA(C)rho1基因敲除小鼠中,通常由GABA(C)受体介导的GABA诱发反应被消除,并且从视杆双极细胞到三级细胞的信号传导发生改变。这些数据表明,通过基因靶向消除GABA(C)rho1亚基会导致视网膜中缺乏GABA(C)受体,并使正常视觉处理过程发生选择性改变。

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