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穿透性角膜移植术和角膜假体植入术对眼后段的影响。

Effect of Penetrating Keratoplasty and Keratoprosthesis Implantation on the Posterior Segment of the Eye.

作者信息

Črnej Alja, Omoto Masahiro, Dohlman Thomas H, Gonzalez-Andrades Miguel, Paschalis Eleftherios I, Cruzat Andrea, Vu T H Khanh, Doorenbos Marianne, Chen Dong Feng, Dohlman Claes H, Dana Reza

出版信息

Invest Ophthalmol Vis Sci. 2016 Apr;57(4):1643-8. doi: 10.1167/iovs.15-17557.

Abstract

PURPOSE

To compare the effects of post-penetrating keratoplasty (PK) and post-keratoprosthesis (KPro) surgery-related inflammation on the posterior segment of the eye and to assess inhibition of tumor necrosis factor alpha (TNFα) and interleukin-1 beta (IL-1β) on these effects.

METHODS

BALB/C (syngeneic) or C57BL/6 (allogeneic) corneas were transplanted onto BALB/C host beds as part of PK or miniature KPro (m-KPro) implantation. Intraocular pressure (IOP) was measured via an intracameral pressure sensor; tissues were harvested and analyzed 8 weeks after surgery. Expression of TNFα and IL-1β in the retina was analyzed using real-time quantitative (q)PCR. Optic nerve degeneration (axon count, circularity, and area) was assessed quantitatively using ImageJ software. After m-KPro implantation, mice were treated with saline, anti-TNFα, or anti-IL-1β antibody, and axonal loss was assessed after 10 weeks.

RESULTS

Mean IOP was within normal limits in the operated and fellow eyes in all groups. The mRNA expression of TNFα and IL-1β was highest in m-KPro groups with either syngeneic or an allogeneic carrier. We observed optic nerve degeneration in both allogeneic PK and m-KPro implanted eyes with an allogeneic carrier. However, TNFα blockade significantly reduced axonal loss by 35%.

CONCLUSIONS

Allogeneic PK and m-KPro implants with an allogeneic carrier lead to chronic inflammation in the posterior segment of the eye, resulting in optic nerve degeneration. In addition, blockade of TNFα prevents axonal degeneration in this preclinical model of allogeneic m-KPro (alloKPro) implantation.

摘要

目的

比较穿透性角膜移植术(PK)和人工角膜植入术(KPro)术后与手术相关的炎症对眼后段的影响,并评估肿瘤坏死因子α(TNFα)和白细胞介素-1β(IL-1β)对这些影响的抑制作用。

方法

将BALB/C(同基因)或C57BL/6(异基因)角膜移植到BALB/C宿主床,作为PK或微型KPro(m-KPro)植入的一部分。通过前房压力传感器测量眼压;术后8周采集组织并进行分析。使用实时定量(q)PCR分析视网膜中TNFα和IL-1β的表达。使用ImageJ软件定量评估视神经变性(轴突计数、圆度和面积)。在植入m-KPro后,用生理盐水、抗TNFα或抗IL-1β抗体治疗小鼠,并在10周后评估轴突损失。

结果

所有组手术眼和对侧眼的平均眼压均在正常范围内。在同基因或异基因载体的m-KPro组中,TNFα和IL-1β的mRNA表达最高。我们在植入异基因载体的异基因PK和m-KPro眼中均观察到视神经变性。然而,TNFα阻断显著减少了35%的轴突损失。

结论

带有异基因载体的异基因PK和m-KPro植入物会导致眼后段慢性炎症,导致视神经变性。此外,在这种异基因m-KPro(alloKPro)植入的临床前模型中,TNFα阻断可防止轴突变性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d737/4829084/a8a2073adb52/i1552-5783-57-4-1643-f01.jpg

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