Retinal safety and toxicity study of artesunate in vitro and in vivo

Bing-Wen Lu , Yu-Xiang Liang , Jin-Feng Liu , Zhong-Qing Sun , Kwok-Fai So , Kin Chiu
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Abstract

Background

Artesunate (ART), a member of the artemisinin family, possesses multi-properties, including anti-inflammation, anti-oxidation, and anti-tumor. ART was recently reported to show anti-neovascularization effect on the cornea, iris, and retina. Compared to the expensive anti-VEGF treatment, this versatile, economical treatment option is attractive in the ophthalmic field. The safety and toxicity profile of ART intravitreal application are in utmost need.

Methods

In this study, immortalized microglial (IMG) cells were treated with ART to determine the safe concentrations without inducing overt inflammatory reactions. Reverse transcription-polymerase chain reaction analysis was used to detect the cytokine expressions in IMG cells in response to ART stimulation. Various doses of ART were intravitreally injected into the right eyes of C57BL/6 mice. Retinal function was tested by electroretinogram, and retinal ganglion cell (RGC) survival was evaluated by counting Brn3a stained cells in flat-mounted retinas at 7 days after ART injection.

Results

ART below 5μM was safe for IMG cells in vitro. Both 2.5 and 5 ​μM ART treatment increased IL-10 gene expression in IMG cells while not changing IL-1β, IL-6, TNF-α, and Arg-1. In the in vivo study, intravitreal injection of ART below 100 ​μM did not cause deterioration in the retinal function and RGC survival of the mouse eyes, while 1 ​mM ART treatment significantly attenuated both the scotopic and photopic b-wave amplitudes and impaired RGC survival. In addition, treatment with ART of 25, 50, and 100 ​μM significantly decreased TNF-α gene expression while ART of 100 ​μM significantly increased IL-10 in the mouse retina.

Conclusions

Intravitreal injection of 100 ​μM ART could downregulate TNF-α while upregulate IL-10 in the mouse retina without causing retinal functional deterioration and RGC loss. ART might be used as anti-inflammatory agent for retinal disorders.

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青蒿琥酯的体内外视网膜安全性及毒性研究
背景青蒿素家族成员Artesunate(ART)具有抗炎、抗氧化、抗肿瘤等多种特性。ART最近被报道对角膜、虹膜和视网膜具有抗新生血管作用。与昂贵的抗VEGF治疗相比,这种多功能、经济的治疗选择在眼科领域具有吸引力。ART玻璃体内应用的安全性和毒性是最需要的。方法对永生化小胶质细胞(IMG)进行ART处理,在不引起明显炎症反应的情况下确定安全浓度。逆转录聚合酶链式反应分析用于检测IMG细胞对ART刺激的细胞因子表达。将不同剂量的ART玻璃体内注射到C57BL/6小鼠的右眼中。通过视网膜电图测试视网膜功能,并通过计数ART注射后7天平板视网膜中Brn3a染色的细胞来评估视网膜神经节细胞(RGC)的存活率。结果5μM以下的ART对体外培养的IMG细胞是安全的。2.5和5​μM ART治疗增加了IMG细胞中IL-10基因的表达,而不改变IL-1β、IL-6、TNF-α和Arg-1。在体内研究中,玻璃体内注射ART低于100​μM不会导致小鼠眼睛的视网膜功能和RGC存活率恶化,而1​mM ART治疗显著减弱了暗视和明视b波振幅,并损害了RGC的存活率。此外,ART治疗25、50和100​μM显著降低TNF-α基因表达,而ART为100​μM显著增加小鼠视网膜中的IL-10。结论100​μM ART可下调小鼠视网膜TNF-α,同时上调IL-10,而不会导致视网膜功能恶化和RGC丧失。ART可能被用作视网膜疾病的抗炎剂。
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来源期刊
CiteScore
1.70
自引率
0.00%
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0
审稿时长
66 days
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