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βB2-晶体蛋白促进成年大鼠损伤视神经的轴突再生。

βB2-Crystallin Promotes Axonal Regeneration in the Injured Optic Nerve in Adult Rats.

作者信息

Böhm Michael R R, Prokosch Verena, Brückner Matthias, Pfrommer Sarah, Melkonyan Harutyun, Thanos Solon

机构信息

Institute for Experimental Ophthalmology, School of Medicine, University of Münster, Albert-Schweitzer-Campus 1, Münster, Germany.

出版信息

Cell Transplant. 2015;24(9):1829-44. doi: 10.3727/096368914X684583. Epub 2014 Oct 8.

Abstract

The purpose of the study was to further scrutinize the potential of βB2-crystallin in supporting regeneration of injured retinal ganglion cell axons both in vitro and in vivo. Retinal explants obtained from animals after treatment either with lens injury (LI) alone or with combined LI 5 days or 3 days before or simultaneously with an optic nerve crush (ONC) were cultured for 96 h under regenerative conditions, and the regenerating axons were quantified and compared with untreated controls. These measurements were then repeated with LI replaced by intravitreal injections of γ-crystallin and β-crystallin at 5 days before ONC. Finally, βB2-crystallin-overexpressing transfected neural progenitor cells (βB2-crystallin-NPCs) in the eye were studied after crushing the optic nerve in vivo. Regeneration was monitored with the aid of immunoblotting of the retina and optic nerve both distal and proximal to the lesion site, and this was compared with controls that received injections of phosphate buffer only. LI performed 5 days or 3 days before ONC significantly promoted axonal outgrowth in vitro (p < 0.001), while LI performed alone before explantation did not. Intravitreal injections of β-crystallin and γ-crystallin mimicked the effects of LI and significantly increased axonal regeneration in culture at the same time intervals (p < 0.001). Western blot analysis revealed that crystallins were present in the proximal optic nerve stump at the lesion site in ONC, but were neither expressed in the undamaged distal optic nerve nor in uninjured tissue. βB2-crystallin-NPCs supported the regeneration of cut optic nerve axons within the distal optic nerve stump in vivo. The reported data suggest that βB2-crystallin-producing "cell factories" could be used to provide novel therapeutic drugs for central nervous system injuries.

摘要

该研究的目的是进一步探究βB2-晶体蛋白在体外和体内支持受损视网膜神经节细胞轴突再生的潜力。从动物身上获取视网膜外植体,这些动物在单独接受晶状体损伤(LI)处理后,或在视神经挤压(ONC)前5天、3天或同时接受LI与ONC联合处理,然后在再生条件下培养96小时,对再生轴突进行定量并与未处理的对照组进行比较。然后,在ONC前5天用玻璃体内注射γ-晶体蛋白和β-晶体蛋白代替LI重复这些测量。最后,在体内对视神经进行挤压后,研究眼中过表达βB2-晶体蛋白的转染神经祖细胞(βB2-晶体蛋白-NPCs)。借助对损伤部位远端和近端的视网膜和视神经进行免疫印迹来监测再生情况,并将其与仅接受磷酸盐缓冲液注射的对照组进行比较。在ONC前5天或3天进行LI显著促进了体外轴突生长(p<0.001),而在植入前单独进行LI则没有这种效果。玻璃体内注射β-晶体蛋白和γ-晶体蛋白模拟了LI的作用,并在相同时间间隔显著增加了培养物中的轴突再生(p<0.001)。蛋白质印迹分析显示,晶体蛋白存在于ONC损伤部位的近端视神经残端,但在未受损的远端视神经和未受伤组织中均未表达。βB2-晶体蛋白-NPCs在体内支持远端视神经残端内切断的视神经轴突的再生。报道的数据表明,产生βB2-晶体蛋白的“细胞工厂”可用于为中枢神经系统损伤提供新型治疗药物。

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