The Mechanisms of Neuroprotection by Topical Rho Kinase Inhibition in Experimental Mouse Glaucoma and Optic Neuropathy.

IF 5 2区 医学 Q1 OPHTHALMOLOGY
Sarah E Quillen, Elizabeth C Kimball, Kelsey A Ritter-Gordy, Liya Du, Zhuochen Yuan, Mary E Pease, Salaheddine Madhoun, Thao D Nguyen, Thomas V Johnson, Harry A Quigley, Ian F Pitha
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引用次数: 0

Abstract

Purpose: The purpose of this study was to delineate the neuroprotective mechanisms of topical 2% ripasudil (Rip), a Rho kinase (ROCK) inhibitor.

Methods: In 340 mice, scheduled 2% Rip or balanced salt solution (BSS) saline drops were intermittently, unilaterally delivered. Intracameral microbead glaucoma (GL) injection increased intraocular pressure (IOP) from 1 day to 6 weeks (6W), whereas other mice underwent optic nerve (ON) crush. Retinal ganglion cell (RGC) loss was assessed using retinal wholemount anti-RNA Binding Protein with Multiple Splicing (RBPMS) labeling and ON axon counts. Axonal transport was quantified with β-amyloid precursor protein (APP) immunolocalization. Micro-Western (Wes) analysis quantified protein expression. Immunofluorescent expression of ROCK pathway molecules, quantitative astrocyte structural changes, and ON biomechanical strains (explanted eyes) were evaluated. ROCK activity assays were conducted in separate ON regions.

Results: At 6W GL, mean RGC axon loss was 6.6 ± 13.3% in Rip and 36.3 ± 30.9% in BSS (P = 0.04, n = 10/group). RGC soma loss after crush was lower with Rip (68.6 ± 8.2%) than BSS (80.5 ± 5.7%, P = 0.006, n = 10/group). After 6W GL, RGC soma loss was lower with Rip (34 ± 5.0%) than BSS (51 ± 8.1%, P = 0.03, n = 10/group). Axonal transport of APP within the unmyelinated ON (UON) was unaffected by Rip. Maximum principal mechanical strains increased similarly in Rip and BSS-treated mice. Retinal ROCK 1 and 2 activity was reduced by Rip in GL eyes. The pROCK2/ROCK2 protein ratio rose in the retina of BSS GL eyes, but not in Rip GL eyes.

Conclusions: Topical Rip reduced RGC loss in GL and ON crush, with suppression of ROCK signaling in the retina and ON. The neuroprotection mechanisms appear to involve effects on both RGC and astrocyte responses to IOP elevation.

局部 Rho 激酶抑制剂在实验性小鼠青光眼和视神经病变中的神经保护机制
目的:本研究旨在阐明 Rho 激酶(ROCK)抑制剂 2% 瑞帕地尔(Rip)的神经保护机制:在 340 只小鼠中,间歇性单侧滴入 2% Rip 或平衡盐溶液(BSS)生理盐水。巩膜内微珠青光眼(GL)注射增加了小鼠1天至6周(6W)的眼内压(IOP),而其他小鼠则接受了视神经(ON)挤压。视网膜神经节细胞(RGC)的损失是通过视网膜整装抗RNA结合蛋白多重剪接(RBPMS)标记和视神经轴突计数来评估的。轴突运输通过β-淀粉样前体蛋白(APP)免疫定位进行量化。显微西法(Wes)分析量化了蛋白质的表达。对 ROCK 通路分子的免疫荧光表达、定量星形胶质细胞结构变化和 ON 生物力学应变(摘除眼球)进行了评估。在不同的ON区域进行了ROCK活性检测:在 6W GL 时,Rip 和 BSS 的 RGC 轴突平均损失率分别为 6.6 ± 13.3% 和 36.3 ± 30.9%(P = 0.04,n = 10/组)。挤压后的 RGC 体节损失,Rip(68.6 ± 8.2%)低于 BSS(80.5 ± 5.7%,P = 0.006,n = 10/组)。在 6W GL 之后,RGC 体节丢失率 Rip(34 ± 5.0%)低于 BSS(51 ± 8.1%,P = 0.03,n = 10/组)。未髓鞘化 ON(UON)内 APP 的轴突运输不受 Rip 的影响。在 Rip 和 BSS 处理的小鼠中,最大主要机械应变的增加情况相似。Rip 降低了 GL 眼睛视网膜 ROCK 1 和 2 的活性。BSS GL眼视网膜中pROCK2/ROCK2蛋白比率上升,而Rip GL眼则没有:结论:外用 Rip 可减少 GL 和 ON 挤压中 RGC 的损失,同时抑制视网膜和 ON 中的 ROCK 信号传导。神经保护机制似乎涉及 RGC 和星形胶质细胞对眼压升高的反应。
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来源期刊
CiteScore
6.90
自引率
4.50%
发文量
339
审稿时长
1 months
期刊介绍: Investigative Ophthalmology & Visual Science (IOVS), published as ready online, is a peer-reviewed academic journal of the Association for Research in Vision and Ophthalmology (ARVO). IOVS features original research, mostly pertaining to clinical and laboratory ophthalmology and vision research in general.
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