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Invest Ophthalmol Vis Sci. 2020 Feb 7;61(2):16. doi: 10.1167/iovs.61.2.16.
Mesopic flash electroretinography (fERG) as a tool to identify N-methyl-d-aspartate receptor (NMDAR) hypofunction in subjects with schizophrenia shows great potential. We report the first fERG study in a genetic mouse model of schizophrenia characterized by NMDAR hypofunction from gene silencing of serine racemase (SR) expression (SR-/-), an established risk gene for schizophrenia. We analyzed fERG parameters under various background light adaptations to determine the most significant variables to allow for early identification of people at risk for schizophrenia, prior to onset of psychosis. SR is a risk gene for schizophrenia, and negative and cognitive symptoms antedate the onset of psychosis that is required for diagnosis.
The scotopic, photopic, and mesopic fERGs were analyzed in male and female mice in both SR-/- and wild-type (WT) mice and also analyzed for sex differences. Amplitude and implicit time of the a- and b-wave components, b-/a-wave ratio, and Fourier transform analysis were analyzed.
Mesopic a- and b-wave implicit times were significantly delayed, and b-wave amplitudes, b/a ratios, and Fourier transform were significantly decreased in the male SR-/- mice compared to WT, but not in female SR-/- mice. No significant differences were observed in photopic or scotopic fERGs between genotype.
The fERG prognostic capability may be improved by examination of background light adaptation, a larger array of light intensities, considering sex as a variable, and performing Fourier transform analyses of all waveforms. This should improve the ability to differentiate between controls and subjects with schizophrenia characterized by NMDAR hypofunction.
作为一种识别精神分裂症患者 N-甲基-D-天冬氨酸受体(NMDAR)功能低下的工具,中间光闪烁视网膜电图(fERG)具有很大的潜力。我们报告了第一个使用 NMDAR 功能低下的遗传精神分裂症小鼠模型进行的 fERG 研究,该模型通过丝氨酸消旋酶(SR)表达基因沉默(SR-/-)表现出 NMDAR 功能低下,SR 是精神分裂症的一个既定风险基因。我们分析了各种背景光适应下的 fERG 参数,以确定最显著的变量,以便在精神病发作前,尽早识别有精神分裂症风险的人群。SR 是精神分裂症的一个风险基因,阴性和认知症状先于需要诊断的精神病发作。
分析了雄性和雌性 SR-/-和野生型(WT)小鼠的暗适应、明适应和中间光 fERG,并分析了性别差异。分析了 a-和 b-波成分的振幅和潜伏期、b-/a-波比和傅里叶变换分析。
与 WT 相比,雄性 SR-/-小鼠的中间光 a-和 b-波潜伏期明显延迟,b-波振幅、b/a 比和傅里叶变换明显降低,但雌性 SR-/-小鼠则不然。在光适应和暗适应 fERG 中,基因型之间没有观察到显著差异。
通过检查背景光适应、更多的光强度、将性别作为变量以及对所有波形进行傅里叶变换分析,fERG 的预后能力可能会得到改善。这应该能够提高区分 NMDAR 功能低下的精神分裂症患者和对照者的能力。