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碘乙酸模型可使猪视网膜选择性出现节段性变性和部分锥体失活。

Selective rod degeneration and partial cone inactivation characterize an iodoacetic acid model of Swine retinal degeneration.

机构信息

Departments of Ophthalmology and Visual Sciences, University of Louisville Health Sciences Center, Kentucky, USA.

出版信息

Invest Ophthalmol Vis Sci. 2011 Oct 7;52(11):7917-23. doi: 10.1167/iovs.11-7849.

Abstract

PURPOSE. Transgenic pigs carrying a mutant human rhodopsin transgene have been developed as a large animal model of retinitis pigmentosa (RP). This model displays some key features of human RP, but the time course of disease progression makes this model costly, time consuming, and difficult to study because of the size of the animals at end-stage disease. Here, the authors evaluate an iodoacetic acid (IAA) model of photoreceptor degeneration in the pig as an alternative model that shares features of the transgenic pig and human RP. METHODS. IAA blocks glycolysis, thereby inhibiting photoreceptor function. The effect of the intravenous injection of IAA on swine rod and cone photoreceptor viability and morphology was followed by histologic evaluation of different regions of the retina using hematoxylin and eosin and immunostaining. Rod and cone function was analyzed by full-field electroretinography and multifocal electroretinography. RESULTS. IAA led to specific loss of rods in a central-to-peripheral retinal gradient. Although cones were resistant, they showed shortened outer segments, loss of bipolar cell synaptic connections, and a diminished flicker ERG, hallmarks of transition to cone dysfunction in RP patients. CONCLUSIONS. IAA provides an alternative rod-dominant model of retinal damage that shares a surprising number of features with the pig transgenic model of RP and with human RP. This IAA model is cost-effective and rapid, ensuring that the size of the animals does not become prohibitive for end-stage evaluation or therapeutic intervention.

摘要

目的。携带突变型人视紫红质转基因的转基因猪已被开发为视网膜色素变性 (RP) 的大型动物模型。该模型显示了一些人类 RP 的关键特征,但由于疾病终末期动物的体型较大,疾病进展的时间过程使该模型成本高、耗时且难以研究。在这里,作者评估了碘乙酸 (IAA) 诱导的光感受器变性模型作为一种替代模型,该模型具有转基因猪和人类 RP 的共同特征。

方法。IAA 阻断糖酵解,从而抑制光感受器功能。通过对视网膜不同区域进行苏木精和伊红染色和免疫染色的组织学评估,跟踪 IAA 静脉注射对猪视杆和视锥光感受器存活和形态的影响。通过全视野视网膜电图和多焦视网膜电图分析视杆和视锥功能。

结果。IAA 导致 rods 以中央到周边的视网膜梯度特异性丧失。尽管 cones 具有抗性,但它们显示出较短的外节段、双极细胞突触连接的丧失以及闪烁 ERG 的减少,这些都是 RP 患者向 cone 功能障碍过渡的标志。

结论。IAA 提供了一种替代的以 rods 为主的视网膜损伤模型,与 RP 的转基因猪模型和人类 RP 具有惊人数量的共同特征。这种 IAA 模型具有成本效益且快速,确保动物的体型不会成为终末期评估或治疗干预的障碍。

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