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评价载苦参碱聚乙二醇酸纳米粒治疗干眼症的疗效。

Evaluating the Efficacy of Polyglycolic Acid-Loading Tetrandrine Nanoparticles in the Treatment of Dry Eye.

机构信息

Department of Ophthalmology, The Second Affiliated Hospital of Chongqing Medical University, Chongqing, China.

Chongqing Key Laboratory of Ultrasound Molecular Imaging, The Second Affiliated Hospital of Chongqing Medical University, Chongqing, China.

出版信息

Ophthalmic Res. 2023;66(1):1148-1158. doi: 10.1159/000533345. Epub 2023 Sep 8.

Abstract

INTRODUCTION

Dry eye disease (DED) is a multifactor-induced disease accompanied by increased osmolarity of the tear film and inflammation of the ocular surface. Traditional anti-inflammation agent corticosteroids applied in DED treatment could result in high intraocular pressure, especially in long-term treatment. Therefore, we explored a nano drug that aimed to block the formation pathway of DED which had anti-inflammatory, sustained release, and good biocompatibility characteristics in this study.

METHODS

We prepared a novel nanomedicine (Tet-ATS@PLGA) by the thin film dispersion-hydration ultrasonic method and detected its nanostructure, particle size, and zeta potential. Flow cytometry was used to detect the cell survival rate of each group after 24 h of drug treatment on inflammed Statens Seruminstitut Rabbit Corneal (SIRC) cells. Observed and recorded corneal epithelial staining, tear film rupture time, and Schirmer test to detect tear secretion on the ocular surface of rabbits. The corneal epithelial thickness, morphology, and number of bulbar conjunctival goblet cells were recorded by H&E staining. Finally, we detected the expression of VEGF, IL-1β, PGE2, and TNF-α by cellular immunofluorescence staining and enzyme-linked immunosorbent assay (ELISA).

RESULTS

The encapsulation efficiency and drug loading of Tet-ATS@PLGA were 79.85% and 32.47%, respectively. At eye surface temperature, Tet can easily release from Tet-ATS@PLGA while that it was difficult to release at storage temperature and room temperature. After 2 weeks medication, Tet-ATS@PLGA can effectively improve the tear film rupture time and tear secretion time in a DED model (p <0.05). Compared with the normal group (62.34 ± 4.86 mm), the thickness of corneal epithelium in ATS (29.47 ± 3.21 mm), Tet-ATS (46.23 ± 2.87 mm), and Tet-ATS@PLGA (55.76 ± 3.95 mm) gradually increased. Furthermore, the flow cytometry indicated that Tet-ATS@PLGA can effectively promote the apoptosis of inflammatory SIRC cells, and the cellular immunofluorescence and ELISA experiments showed that the expression intensity of inflammatory factors such as VEGF, IL-1β, PGE2, and TNF-α decreased in this process. Interestingly, Tet also had the effect of reducing intraocular pressure.

CONCLUSION

Tet-ATS@PLGA can effectively promote the apoptosis of inflammatory corneal epithelial cells, thus inhibiting the expression of inflammatory factors to block the formation of DED and improve the secretion of tear on the ocular surface.

摘要

简介

干眼疾病(DED)是一种多因素诱导的疾病,伴有泪膜渗透压升高和眼表面炎症。传统的抗炎药物皮质类固醇在 DED 治疗中可导致眼内压升高,尤其是在长期治疗中。因此,我们在这项研究中探索了一种旨在阻断 DED 形成途径的纳米药物,该药物具有抗炎、持续释放和良好的生物相容性特点。

方法

我们通过薄膜分散-水合超声法制备了一种新型纳米药物(Tet-ATS@PLGA),并检测了其纳米结构、粒径和 Zeta 电位。通过流式细胞术检测药物处理 24 小时后各组对 Statens Seruminstitut Rabbit Corneal(SIRC)细胞的细胞存活率。观察并记录兔眼表面角膜上皮染色、泪膜破裂时间和 Schirmer 试验以检测泪液分泌。通过 H&E 染色记录角膜上皮厚度、形态和球结膜杯状细胞数量。最后,通过细胞免疫荧光染色和酶联免疫吸附试验(ELISA)检测 VEGF、IL-1β、PGE2 和 TNF-α的表达。

结果

Tet-ATS@PLGA 的包封效率和载药量分别为 79.85%和 32.47%。在眼表面温度下,Tet 很容易从 Tet-ATS@PLGA 中释放,而在储存温度和室温下则很难释放。经过 2 周的药物治疗,Tet-ATS@PLGA 可有效改善 DED 模型中的泪膜破裂时间和泪液分泌时间(p <0.05)。与正常组(62.34 ± 4.86 mm)相比,ATS(29.47 ± 3.21 mm)、Tet-ATS(46.23 ± 2.87 mm)和 Tet-ATS@PLGA(55.76 ± 3.95 mm)组的角膜上皮厚度逐渐增加。此外,流式细胞术表明 Tet-ATS@PLGA 能有效促进炎症 SIRC 细胞的凋亡,细胞免疫荧光和 ELISA 实验表明,VEGF、IL-1β、PGE2 和 TNF-α 等炎症因子的表达强度在这一过程中降低。有趣的是,Tet 还有降低眼压的作用。

结论

Tet-ATS@PLGA 能有效促进炎症性角膜上皮细胞凋亡,从而抑制炎症因子的表达,阻断 DED 的形成,改善眼表面的泪液分泌。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d566/10614459/a5de6fa41893/ore-2023-0066-0001-533345_F01.jpg

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