Laboratory of Immunology, National Eye Institute, National Institutes of Health, Bethesda, MD, USA.
J Neuroinflammation. 2012 Mar 27;9:59. doi: 10.1186/1742-2094-9-59.
Inflammatory responses are detected in the retina of patients with age-related macular degeneration and Ccl2-/-/Cx3cr1-/- mice on rd8 background,(Ccl2-/-/Cx3cr1-/- mice) a model that develops progressive age-related macular degeneration-like retinal lesions including focal photoreceptor degeneration, abnormal retinal pigment epithelium and A2E accumulation. Tumor necrosis factor-inducible gene 6 protein is an anti-inflammatory protein and has been shown to improve myocardial infarction outcome and chemically injured cornea in mice by suppressing inflammation. In this study, we evaluated the effect of an intravitreous injection of recombinant TSG-6 on the retinal lesions of Ccl2-/-/Cx3cr1-/- mice.
Recombinant TSG-6 (400 ng) was administered by intravitreous injection into the right eye of six-week-old Ccl2-/-/Cx3cr1-/- mice. Their left eye was injected with phosphate-buffered saline as a control. Funduscopic pictures were taken before injection and sequentially once a month after injection. The mice were killed two months after injection and the ocular histology examined. Retinal A2E, a major component of lipofuscin, was measured by high performance liquid chromatography. The microarray of ocular mRNA of 92 immunological genes was performed. The genes showing differentiated expression in microarray were further compared between the injected right eye and the contralateral (control) eye by [real-time quantitative reverse transcription polymerase chain reaction] qRT-PCR.
The continuous monitoring of the fundus for two months showed a slower progression or alleviation of retinal lesions in the treated right eyes as compared with the untreated left eyes. Among 23 pairs of eyes, the lesion levels improved in 78.3%, stayed the same in 8.7% and progressed in 13.0%. Histology confirmed the clinical observation. Even though there was no difference in the level of A2E between the treated and the untreated eyes, microarray analysis of 92 immune genes showed that IL-17a was substantially decreased after the treatment. Expression of TNF-α showed a similar pattern to IL-17a. The results were consistent in duplicated arrays and confirmed by qRT-PCR.
We concluded that intravitreous administration of recombinant TSG-6 might stabilize retinal lesions in Ccl2-/-/Cx3cr1-/- mice on rd8 background. Modulation of ocular immunological gene expressions, especially IL-17a, could be one of the mechanisms.
在年龄相关性黄斑变性患者的视网膜和 rd8 背景下的 Ccl2-/-/Cx3cr1-/-小鼠(Ccl2-/-/Cx3cr1-/- 小鼠)中检测到炎症反应,Ccl2-/-/Cx3cr1-/- 小鼠是一种发展为进行性年龄相关性黄斑变性样视网膜病变的模型,包括局灶性光感受器变性、异常视网膜色素上皮和 A2E 积累。肿瘤坏死因子诱导基因 6 蛋白是一种抗炎蛋白,已被证明通过抑制炎症来改善心肌梗死和化学损伤的小鼠的结果角膜。在这项研究中,我们评估了玻璃体内注射重组 TSG-6 对 Ccl2-/-/Cx3cr1-/- 小鼠视网膜病变的影响。
将重组 TSG-6(400ng)通过玻璃体内注射到六周龄 Ccl2-/-/Cx3cr1-/- 小鼠的右眼。左眼注射磷酸盐缓冲盐水作为对照。在注射前和注射后每月一次拍摄眼底照片。注射后两个月处死小鼠并检查眼部组织学。通过高效液相色谱法测量视网膜 A2E,A2E 是脂褐素的主要成分。进行了 92 个免疫基因的眼部 mRNA 微阵列分析。通过 [实时定量逆转录聚合酶链反应] qRT-PCR 进一步比较了注射右眼与对侧(对照)眼之间微阵列中表达差异的基因。
连续两个月监测眼底显示,与未经治疗的左眼相比,治疗右眼的视网膜病变进展较慢或缓解。在 23 对眼睛中,78.3%的病变程度改善,8.7%的病变程度保持不变,13.0%的病变程度进展。组织学检查证实了临床观察结果。尽管治疗眼和未治疗眼之间的 A2E 水平没有差异,但对 92 个免疫基因的微阵列分析表明,IL-17a 治疗后明显减少。TNF-α 的表达模式与 IL-17a 相似。重复数组的结果一致,并通过 qRT-PCR 得到证实。
我们得出的结论是,玻璃体内注射重组 TSG-6 可能稳定 rd8 背景下 Ccl2-/-/Cx3cr1-/- 小鼠的视网膜病变。眼免疫基因表达的调节,特别是 IL-17a,可能是其中一种机制。
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