将 AAV2 基因植入猫视网膜神经节细胞。

IF 1.5 4区心理学 Q4 NEUROSCIENCES

Vision Research Pub Date : 2024-11-16 DOI:10.1016/j.visres.2024.108519

Kazuya Oikawa , J.Seth Eaton , Julie A. Kiland , Odalys Torné , Virginia Mathu , Robert W. Nickells , Gillian J. McLellan

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引用次数: 0

摘要

在治疗青光眼的过程中，神经保护和保留视网膜神经节细胞（RGC）的有效策略仍然难以捉摸。在猫身上发现了一种自发的青光眼遗传模型，并将其广泛表征为一种可行的转化模型，其眼睛大小和解剖结构与人类相似。在这项研究中，我们试图在正常猫体内通过玻璃体内注射 AAV2 将基因传递到猫的 RGCs，并对这一概念进行初步验证。我们在 5 只成年猫的中央区上方进行了 AAV2/2-CMV-GFP 视网膜前、后玻璃体内注射。围手术期口服泼尼松龙进行免疫抑制，并在注射后 6-10 周内逐渐减量。注射前后均进行了眼科检查。在6-10周内，每隔1-2周分别使用共焦扫描激光眼底镜（cSLO）和光学相干断层扫描（OCT）（Spectralis OCT-HRA，海德堡）监测GFP报告表达和病毒转导对视网膜的形态学影响。在基线和注射后记录全场视网膜电图（ERG）和视觉诱发电位（VEP）。通过组织学和免疫标记RGC标记物RBPMS及Müller细胞和星形胶质细胞标记物SOX9检查视网膜，并检查视网膜、视神经（ON）、视束和外侧膝状核（LGN）中的GFP表达。注射后1-2周，通过cSLO观察GFP+视网膜细胞和RGC轴突。活体 OCT 未观察到视网膜形态学变化，但有 3/5 的眼睛在组织学上表现出轻微的视网膜炎症。与基线和未处理的眼睛相比，注射眼的视网膜和视网膜功能都得到了保留。GFP 主要在 RBPMS+ RGC 细胞和 SOX9+ Müller 细胞中表达。在中央视觉通路的整个 RGC 神经纤维束中都能观察到 GFP 荧光。在 GFP 高表达区域观察到 RGC 的峰值转导（高达 ∼ 20 %），但在 GFP 低表达区域观察到 RGC 的峰值转导（高达 ∼ 20 %）。

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Intravitreal AAV2 gene delivery to feline retinal ganglion cells

Effective strategies for the neuroprotection and preservation of retinal ganglion cells (RGCs) remain elusive in the management of glaucoma. A spontaneous genetic model of glaucoma has been identified in cats and extensively characterized as a viable translational model, with eye size and anatomy similar to humans. In this study we sought to establish initial proof of concept for gene delivery to feline RGCs via intravitreal injection of AAV2 in normal cats. Pre-retinal, posterior vitreal injection of AAV2/2-CMV-GFP, was performed overlying the area centralis in 5 adult cats. Immunosuppressive oral prednisolone was administered perioperatively and gradually tapered over 6-10wks post-injection. Ophthalmic examination was performed pre- and post-injection. The GFP reporter expression and morphological effects of viral transduction on the retina were monitored in vivo using confocal scanning laser ophthalmoscopy (cSLO) and optical coherence tomography (OCT), respectively (Spectralis OCT-HRA, Heidelberg), at 1-2wk intervals over 6-10wks. Full-field electroretinograms (ERG) and visual evoked potentials (VEP) were recorded at baseline and post-injection. Retinas were examined by histology and immunolabeling for the RGC marker RBPMS and Müller cell and astrocyte marker SOX9, and GFP expression was examined in the retina, optic nerve (ON), optic tract and lateral geniculate nucleus (LGN). GFP⁺ retinal cells and RGC axons were visualized by cSLO at 1–2 weeks post-injection. No retinal morphological changes were observed by OCT in vivo but 3/5 eyes exhibited mild retinal inflammation on histology. Retinal and ON function were preserved in injected eyes compared to baseline and untreated eyes. GFP expression was predominantly identified in RBPMS⁺ RGC cells as well as SOX9⁺ Müller cells. GFP fluorescence was observed throughout RGC nerve fiber tract in the central visual pathway. Peak transduction in RGCs (up to ∼ 20 %) was observed in the regions with high GFP expression, but < 1 % of RGCs expressed GFP across the whole retina. Our data provide proof of concept that pre-retinal injection of AAV2/2 may represent a feasible platform for gene delivery to feline RGCs in vivo but highlight a need for further refinement to improve RGC transduction efficiency and control low-grade retinal inflammation.

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来源期刊

Vision Research 医学-神经科学

CiteScore

3.70

自引率

16.70%

发文量

111

审稿时长

66 days

期刊介绍： Vision Research is a journal devoted to the functional aspects of human, vertebrate and invertebrate vision and publishes experimental and observational studies, reviews, and theoretical and computational analyses. Vision Research also publishes clinical studies relevant to normal visual function and basic research relevant to visual dysfunction or its clinical investigation. Functional aspects of vision is interpreted broadly, ranging from molecular and cellular function to perception and behavior. Detailed descriptions are encouraged but enough introductory background should be included for non-specialists. Theoretical and computational papers should give a sense of order to the facts or point to new verifiable observations. Papers dealing with questions in the history of vision science should stress the development of ideas in the field.