遗传性视网膜营养不良的视网膜内功能。

Acta anatomica Pub Date : 1998-01-01 DOI:10.1159/000046483
K Ruether, U Kellner
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引用次数: 20

摘要

遗传性视网膜营养不良是最常见的光感受器和/或视网膜色素上皮的疾病。继发于光感受器层的结构,如双极、水平、无突细胞和神经节细胞继发参与。在该疾病的晚期,会发生轻度至中度的内视网膜丧失,但即使在视网膜营养不良的晚期和严重阶段,第二和第三神经元也令人惊讶地保持活力。遗传性视网膜营养不良患者的内视网膜功能不容易确定,因为它依赖于光感受器的输入。视网膜电图(ERG)在这方面提供了几种可能性:b波,off-response (off-ERG),振荡电位,闪烁ERG和模式ERG的暗阈值响应(PERG)。我们看了两个ERG测试:PERG和off-ERG。PERG是神经节细胞功能的指标。其振幅与由闪光ERG和视野测试确定的光感受器输入有关。但在无法检测到的闪光ERG反应的情况下,PERG可以在一些患者中记录下来,而在其他患者中则不能。这可能表明不同组的患者对视网膜内功能有不同的影响。打开和关闭反应与去极化和超极化双极细胞的功能有关。对301例各种视网膜营养不良患者的评估显示,大多数遗传性疾病主要影响光感受器或色素上皮。在一些患者中,开启和关闭反应幅度或内隐时间的改变表明视网膜内病变和不同的病理生理机制。然而,必须仔细解释,因为打开和关闭反应可能受到双极细胞、双极细胞、m ller细胞和细胞间基质的感光突触功能障碍的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inner retinal function in hereditary retinal dystrophies.

Hereditary retinal dystrophies are most often disorders of photoreceptors and/or the retinal pigment epithelium. Structures secondary to the photoreceptor layer such as bipolar, horizontal, amacrine and ganglion cells are secondarily involved. In later stages of the disease a mild to moderate loss of inner retina occurs, but the second and third neurons remain surprisingly viable even in late and severe stages of retinal dystrophies. The function of the inner retina in patients suffering from hereditary retinal dystrophies is not easy to determine because it depends on the input of photoreceptors. The electroretinogram (ERG) offers several possibilities in this respect: b-wave, off-response (off-ERG), oscillatory potentials, scotopic threshold response of the flash ERG and the pattern ERG (PERG). We looked at two ERG tests: the PERG and the off-ERG. The PERG is an indicator of ganglion cell function. Its amplitude is related to the photoreceptor input determined by the flash ERG and visual field testing. But in cases of an undetectable flash ERG response the PERG can be recorded in some patients, but not in others. This may be an indication of a different effect on inner retinal function in different groups of patients. On- and off-responses are related to the function of depolarizing and hyperpolarizing bipolar cells. Evaluation of 301 patients with various retinal dystrophies revealed that most hereditary disorders primarily affect the photoreceptors or the pigment epithelium. In some patients, alterations of the on- and off-response amplitudes or implicit times were indicative of inner retinal disorders and different pathophysiologic mechanisms. However, interpretation has to be made carefully, as on- and off-responses may be influenced by dysfunction of photoreceptor synapses to bipolar cells, bipolar cells, Müller cells and intercellular matrix.

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