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首页> 外文期刊>Investigative ophthalmology & visual science >Sustained Subconjunctival Delivery of Infliximab Protects the Cornea and Retina Following Alkali Burn to the Eye
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Sustained Subconjunctival Delivery of Infliximab Protects the Cornea and Retina Following Alkali Burn to the Eye

机译:英夫利昔单抗的结膜下持续递送可保护碱烧至眼睛后的角膜和视网膜

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Purpose: Tumor necrosis factor (TNF)-?± is upregulated in eyes following corneal alkali injury and contributes to corneal and also retinal damage. Prompt TNF-?± inhibition by systemic infliximab ameliorates retinal damage and improves corneal wound healing. However, systemic administration of TNF-?± inhibitors carries risk of significant complications, whereas topical eye-drop delivery is hindered by poor ocular bioavailability and the need for patient adherence. This study investigates the efficacy of subconjunctival delivery of TNF-?± antibodies using a polymer-based drug delivery system (DDS). Methods: The drug delivery system was prepared using porous polydimethylsiloxane/polyvinyl alcohol composite fabrication and loaded with 85 ??g of infliximab. Six Dutch-belted pigmented rabbits received ocular alkali burn with NaOH. Immediately after the burn, subconjunctival implantation of anti-TNF-?± DDS was performed in three rabbits while another three received sham DDS (without antibody). Rabbits were followed with photography for 3 months. Results: After 3 months, the device was found to be well tolerated by the host and the eyes exhibited less corneal damage as compared to eyes implanted with a sham DDS without drug. The low dose treatment suppressed CD45 and TNF-?± expression in the burned cornea and inhibited retinal ganglion cell apoptosis and optic nerve degeneration, as compared to the sham DDS treated eyes. Immunolocalization revealed drug penetration in the conjunctiva, cornea, iris, and choroid, with residual infliximab in the DDS 3 months after implantation. Conclusions: This reduced-risk biologic DDS improves corneal wound healing and provides retinal neuroprotection, and may be applicable not only to alkali burns but also to other inflammatory surgical procedures such as penetrating keratoplasty and keratoprosthesis implantation.
机译:目的:角膜碱损伤后眼中的肿瘤坏死因子(TNF)-α±上调,并有助于角膜和视网膜损伤。全身性英夫利昔单抗可迅速抑制TNF-α,改善视网膜损伤并改善角膜伤口愈合。然而,TNF-α±抑制剂的全身给药具有明显并发症的风险,而眼用生物利用度差和需要患者依从性阻碍了局部滴眼剂的递送。这项研究调查了使用基于聚合物的药物递送系统(DDS)结膜下递送TNF-α±抗体的功效。方法:采用多孔聚二甲基硅氧烷/聚乙烯醇复合材料制备药物装载系统,并装载85克g英夫利昔单抗。六只荷兰系带色素的兔子接受了NaOH碱液烧伤。烧伤后立即在三只兔子中进行抗TNF-α±DDS的结膜下植入,而另外三只接受了假DDS(无抗体)。对兔子进行摄影3个月。结果:3个月后,发现该装置对宿主的耐受性良好,与植入无药物的假DDS的眼睛相比,眼睛的角膜损伤更少。与深DDS处理的眼睛相比,低剂量治疗可抑制烧伤角膜中CD45和TNF-α的表达,并抑制视网膜神经节细胞凋亡和视神经变性。免疫定位显示药物在结膜,角膜,虹膜和脉络膜中渗透,植入后3个月DDS中残留英夫利昔单抗。结论:这种降低风险的生物DDS可以改善角膜伤口愈合并提供视网膜神经保护,不仅适用于碱烧伤,而且还适用于其他炎症性外科手术,例如穿透性角膜移植术和角膜移植术。

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