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致癌基因诱导的转基因小鼠视网膜水平细胞变性的功能后果。

Functional consequences of oncogene-induced horizontal cell degeneration in the retinas of transgenic mice.

作者信息

Peachey N S, Roveri L, Messing A, McCall M A

机构信息

Research Service, Hines VA Hospital, IL 60141, USA.

出版信息

Vis Neurosci. 1997 Jul-Aug;14(4):627-32. doi: 10.1017/s0952523800012591.

Abstract

Visual function was evaluated in transgenic mice expressing the simian virus 40 early region under the control of the promoter for phenylethanolamine-N-methyltransferase. These transgenic mice undergo a degeneration of the retinal horizontal cells and the outer plexiform layer. Electroretinograms (ERGs) were recorded under stimulus conditions chosen to elicit both receptoral and postreceptoral responses. The dark-adapted a-waves obtained from transgenic mice were not different from control recordings, indicating that the degenerative process does not interfere with function of the rod photoreceptors. In comparison, the ERG b-wave was markedly reduced in transgenic mice under both dark- and light-adapted conditions. Reproducible visual evoked potentials (VEPs) were recorded from transgenic mice in response to both low luminance stimuli that isolate rod function, and to higher luminance stimuli, indicating that retinal activity is transmitted centrally to the visual cortex. However, VEPs were delayed at all stimulus luminances compared to controls. Analysis of luminance-response functions suggests that the VEP delays could reflect the combination of a decrease in synaptic efficacy and an overall loss in visual sensitivity. These functional abnormalities correlate well with the anatomical abnormalities that have been previously observed in the transgenic retina (Hammang et al., 1993), namely a reduced number of synapses between photoreceptors and second-order neurons.

摘要

在由苯乙醇胺 - N - 甲基转移酶启动子控制下表达猿猴病毒40早期区域的转基因小鼠中评估视觉功能。这些转基因小鼠会经历视网膜水平细胞和外网状层的退化。在选择用于引发感受器和感受器后反应的刺激条件下记录视网膜电图(ERG)。从转基因小鼠获得的暗适应a波与对照记录没有差异,表明退化过程不会干扰视杆光感受器的功能。相比之下,在暗适应和明适应条件下,转基因小鼠的ERG b波均明显降低。在转基因小鼠中记录到了可重复的视觉诱发电位(VEP),其对分离视杆功能的低亮度刺激和更高亮度刺激均有反应,表明视网膜活动可向视觉皮层进行中枢传递。然而,与对照组相比,在所有刺激亮度下VEP均延迟。亮度 - 反应函数分析表明,VEP延迟可能反映了突触效能降低和视觉敏感度整体丧失的综合情况。这些功能异常与先前在转基因视网膜中观察到的解剖学异常(Hammang等人,1993年)密切相关,即光感受器与二级神经元之间的突触数量减少。

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