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玻璃体后脱离联合微纤维蛋白溶解酶可改变兔眼内注射bevacizumab(阿瓦斯汀)的视网膜穿透性。

Posterior vitreous detachment with microplasmin alters the retinal penetration of intravitreal bevacizumab (Avastin) in rabbit eyes.

机构信息

Associated Retinal Consultants, Royal Oak, Michigan, USA.

出版信息

Retina. 2011 Feb;31(2):393-400. doi: 10.1097/IAE.0b013e3181e586b2.

Abstract

PURPOSE

Intravitreal bevacizumab (BV) (Avastin, Genentech Inc., South San Francisco, CA) is frequently used for the treatment of age-related macular degeneration. Previous studies have demonstrated full-thickness retinal penetration. Intravitreal recombinant microplasmin (MP) has been shown to successfully induce a posterior vitreous detachment (PVD) and vitreous liquefaction in animals. It has been suggested that a PVD may alter the retinal penetration of molecules in the vitreous cavity. The aim of this study was to compare BV retinal penetration in rabbit eyes with and without an MP-induced PVD.

METHODS

Twelve adult rabbits were injected with 0.1 mL (0.4 mg) of MP into the vitreous cavity of 1 eye. One week later, the rabbits were injected with 0.05 mL (1.25 mg) of BV into both eyes. Both eyes of 3 rabbits were harvested at 6 hours, 12 hours, 24 hours, and 72 hours after the BV injection. Frozen retinal cross sections were prepared, and BV retinal penetration was evaluated with immunohistochemistry using a fluorescence-labeled antibody against BV. Two eyes from one rabbit were not injected with either agent and used as controls to compare the background autofluorescence. Peripapillary retinal sections were recorded with a digital camera, and intraretinal BV fluorescence-labeled antibody was measured by qualitative photographic interpretation. Two additional rabbits received an intravitreal injection of 0.1 mL of MP in 1 eye. One week later, both eyes from each rabbit were enucleated, and frozen retinal sections were prepared and analyzed with light microscopy to evaluate histologic damage.

RESULTS

Full-thickness BV retinal penetration was observed throughout the retina in both eyes of each rabbit. All the MP-injected eyes exhibited increased antibody labeling in retinas evaluated at 6 hours, 12 hours, and 24 hours after BV injection when compared with the contralateral non-MP-injected eyes. By 3 days after BV injection, all eyes demonstrated decreased antibody labeling compared with earlier periods. At 3 days, 1 rabbit showed increased antibody labeling in the retina of the non-MP-injected eye compared with the contralateral MP-injected eye, and 2 rabbits exhibited similar antibody labeling in both eyes. When compared with control eyes, light microscopy demonstrated normal retinal histologic findings in eyes injected only with MP.

CONCLUSION

Increased BV retinal penetration is observed initially in eyes with an MP-induced PVD, and the mechanism is likely multifactorial. By 3 days, retinal penetration is similar in eyes with and without a PVD. Although it is difficult to directly extrapolate to humans, our study suggests that a PVD may alter the retinal penetration of BV.

摘要

目的

玻璃体内注射贝伐单抗(BV)(Avastin,基因泰克公司,旧金山,加利福尼亚州)常用于治疗年龄相关性黄斑变性。先前的研究表明它可以完全穿透视网膜。玻璃体内注射重组微纤维蛋白溶酶(MP)已被证明可成功诱导动物的后玻璃体脱离(PVD)和玻璃体液化。有人认为,PVD 可能会改变玻璃体腔中分子的视网膜穿透性。本研究的目的是比较有和没有 MP 诱导的 PVD 的兔眼 BV 的视网膜穿透性。

方法

12 只成年兔的 1 只眼玻璃体内注射 0.1 mL(0.4 mg)MP。1 周后,所有兔子的双眼均注射 0.05 mL(1.25 mg)BV。在 BV 注射后 6 小时、12 小时、24 小时和 72 小时,分别取 3 只兔子的双眼视网膜进行冷冻切片。用荧光标记的 BV 抗体进行免疫组织化学评估,以评估 BV 的视网膜穿透性。一只兔子的两只眼睛均未注射任何药物,用作对照组以比较背景自发荧光。使用数码相机记录视乳头周围视网膜切片,并通过定性摄影解释测量视网膜内 BV 荧光标记抗体。另外 2 只兔子的 1 只眼玻璃体内注射 0.1 mL MP。1 周后,每只兔子的双眼均眼球摘出,制备冷冻视网膜切片,并用光学显微镜进行分析以评估组织学损伤。

结果

在每只兔子的双眼视网膜中均观察到全层 BV 视网膜穿透。与对侧非 MP 注射眼相比,所有接受 MP 注射的眼在 BV 注射后 6 小时、12 小时和 24 小时评估时均表现出增加的抗体标记。在 BV 注射后 3 天,所有眼与早期相比均表现出减少的抗体标记。在 3 天时,1 只兔子的非 MP 注射眼的抗体标记增加,与对侧 MP 注射眼相比,2 只兔子的双眼抗体标记相似。与对照眼相比,仅注射 MP 的眼的光镜检查显示视网膜组织学发现正常。

结论

在 MP 诱导的 PVD 眼中,最初观察到 BV 视网膜穿透增加,其机制可能是多因素的。在 3 天时,PVD 眼和非 PVD 眼的视网膜穿透性相似。尽管很难直接外推到人类,但我们的研究表明 PVD 可能会改变 BV 的视网膜穿透性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8133/3057916/1e0052bd2a01/nihms-221861-f0001.jpg

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