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The BALB/c mouse: Effect of standard vivarium lighting on retinal pathology during aging

机译:BALB / c小鼠:衰老过程中标准玻璃体照明对视网膜病理的影响

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摘要

BALB/cJ mice housed under normal vivarium lighting conditions can exhibit profound retinal abnormalities, including retinal infoldings, autofluorescent inflammatory cells, and photoreceptor degeneration. To explore the sensitivity of the outer retina to cyclic lighting during aging, a cohort of BALB/cJ mice was evaluated with Scanning Laser Ophthalmoscopy (SLO), Spectral-Domain Optical Coherence Tomography (OCT) and conventional histopathology. Mice were bred and reared in a low-illuminance (extracage/intracage: 13 lx/1 lx) vivarium under cyclic light (14 h light: 10 h dark). Retinal imaging (around postnatal day 70) was performed to screen for any pre-existing abnormalities and to establish a baseline. Mice with normal retinas were separated into groups (A, B, C) and placed on bottom (Groups A & B) or top (Group C) of the cage racks where cage illumination was <10 & 150 lx respectively. Experimental groups B & C were imaged multiple times over a 17 month period. Mice from group A (controls) were imaged only once post-baseline at various times for comparison to groups B & C. Mice were assessed by histology at 8, 15, 20, 36, and 56 weeks and immunohistochemistry at 15 weeks post-baseline. SLO and OCT retinal images were measured and the resulting trends displayed as a function of age and light exposure. Retinal lesions (RL) and autofluorescent foci (AFF) were identified with histology as photoreceptor layer infoldings (IF) and localized microglia/macrophages (MM), respectively. Few RL and AFF were evident at baseline. Retinal infoldings were the earliest changes followed by subjacent punctate autofluorescent MM. The colocalization of IF and MM suggests a causal relationship. The incidence of these pathological features increased in all groups relative to baseline. OCT imaging revealed thinning of the outer nuclear layer (ONL) in all groups at 1 year relative to baseline. ONL thinning followed an exponential rate of change but the decay constant varied depending on intensity of illumination of the groups. Advanced age and top row illuminance conditions resulted in significant photoreceptor cell loss as judged by decreased thickness of the ONL. Photoreceptor loss was preceded by both retinal infoldings and the presence of autofluorescent inflammatory cells in the outer retina, suggesting that these changes are early indicators of light toxicity in the BALB/cJ mouse.
机译:在正常饲养箱光照条件下饲养的BALB / cJ小鼠可能会​​表现出严重的视网膜异常,包括视网膜折叠,自体荧光炎性细胞和感光器变性。为了探索衰老过程中外部视网膜对周期性照明的敏感性,通过扫描激光检眼镜(SLO),光谱域光学相干断层扫描(OCT)和常规组织病理学评估了一组BALB / cJ小鼠。在循环光照(14 h光照:10 h黑暗)下,在低照度(吸气/吸气:13 lx / 1 lx)饲养箱中饲养和饲养小鼠。进行视网膜成像(产后第70天左右)以筛查任何先前存在的异常并建立基线。将具有正常视网膜的小鼠分成组(A,B,C),并分别放在笼照明度分别小于10和150 lx的笼架的底部(A和B组)或顶部(C组)。实验组B和C在17个月内多次成像。基线后在不同时间仅对A组(对照组)的小鼠进行一次成像,以与B和C组进行比较。在基线后第8、15、20、36和56周通过组织学评估小鼠,在基线后第15周通过免疫组织化学评估小鼠。测量了SLO和OCT视网膜图像,并显示了随年龄和光照变化的趋势。视网膜病变(RL)和自发荧光灶(AFF)在组织学上分别被识别为感光层折叠(IF)和局部小胶质细胞/巨噬细胞(MM)。在基线时,很少有RL和AFF明显。视网膜褶皱是最早的变化,其次是点状点状自发荧光MM。 IF和MM的共定位表明有因果关系。相对于基线,所有组中这些病理特征的发生率均增加。 OCT成像显示,相对于基线,所有组在1年时外核层(ONL)变薄。 ONL稀化遵循指数变化率,但是衰减常数根据组的照明强度而变化。老年和顶行照度条件导致显着的感光细胞损失,这可以通过减少ONL的厚度来判断。视网膜折叠和外部视网膜中自体荧光炎细胞的存在都导致光感受器丧失,这表明这些变化是BALB / cJ小鼠光毒性的早期指标。

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