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Neuroprotective vaccination with copolymer-1 decreases laser-induced retinal damage

机译:共聚物1的神经保护性疫苗接种减少了激光诱导的视网膜损伤

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The retinal damage induced by laser photocoagulation increases manifold by the secondary degeneration process whereby tissues adjacent to the primary lesion are destroyed. The neuroprotective effect of immunization by glatiramer acetate (Copolymer-1, Cop-1) in adjuvant was previously demonstrated in models of retina, optic nerve, brain, and spinal cord lesions. The present study tested the neuroprotective ability of Cop-1 to reduce the spread of laser-induced retinal damage. Standard argon laser lesions were created in 72 DA pigmented rats divided into four groups: two Cop-1 treated groups (animals treated seven days before or immediately after the laser session) and two control groups treated respectively by saline or the effective but toxic neuroprotective compound MK-801. The histological and morphological evaluations of the lesions 3, 20, and 60 days after the injury revealed significant reduction in photoreceptor loss of the retinas of the pre-immunized animals. Cop-1 given after the laser injury did not prevent cell loss significantly, while the neuroprotective effect of MK-801 was observed only on the third day after the laser injury. The results show that pre-immunization with Cop-1 is neuroprotective in unmyelinated (gray matter) neural tissue such as the retina. This approach may be of clinical significance in ameliorating laser-induced retinal injuries in humans.
机译:激光光凝引起的视网膜损伤通过继发性变性过程而增加了多种,从而破坏了与原发性病变相邻的组织。醋酸格拉替雷(Copolymer-1,Cop-1)在佐剂中免疫的神经保护作用先前已在视网膜,视神经,脑和脊髓损伤模型中得到证实。本研究测试了Cop-1的神经保护能力,以减少激光诱导的视网膜损伤的扩散。在72只DA色素染成的大鼠中创建标准的氩激光损伤,分为四组:两个Cop-1治疗组(在激光治疗之前或之后立即治疗的动物)和两个对照组分别用生理盐水或有效但有毒的神经保护化合物治疗MK-801。损伤后3、20和60天的病变的组织学和形态学评估显示,预免疫动物视网膜的感光细胞损失显着减少。激光损伤后给予的Cop-1不能明显防止细胞丢失,而仅在激光损伤后的第三天才观察到MK-801的神经保护作用。结果表明,用Cop-1进行的预免疫在无髓(灰质)神经组织(如视网膜)中具有神经保护作用。这种方法在减轻激光对人的视网膜损伤中可能具有临床意义。

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