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OTX2刺激成年视网膜神经节细胞再生。

OTX2 stimulates adult retinal ganglion cell regeneration.

作者信息

Ibad Raoul Torero, Quenech'du Nicole, Prochiantz Alain, Moya Kenneth L

机构信息

Univ. Lille, CNRS, UMR 8523 - PhLAM - Physique des Lasers Atomes et Molécules, F-59000 Lille, France.

Centre for Interdisciplinary Research in Biology (CIRB), Collége de France, CNRS UMR 7241, INSERM U1050, Labex MemoLife, Paris Sciences et Lettres Research University, Paris, France.

出版信息

Neural Regen Res. 2022 Mar;17(3):690-696. doi: 10.4103/1673-5374.320989.

Abstract

Retinal ganglion cell (RGC) axons provide the only link between the light sensitive and photon transducing neural retina and visual centers of the brain. RGC axon degeneration occurs in a number of blinding diseases and the ability to stimulate axon regeneration from surviving ganglion cells could provide the anatomic substrate for restoration of vision. OTX2 is a homeoprotein transcription factor expressed in the retina and previous studies showed that, in response to stress, exogenous OTX2 increases the in vitro and in vivo survival of RGCs. Here we examined and quantified the effects of OTX2 on adult RGC axon regeneration in vitro and in vivo. The results show that exogenous OTX2 stimulates the regrowth of axons from RGCs in cultures of dissociated adult retinal cells and from explants of adult retinal tissue and that RGCs respond directly to OTX2 as regrowth is observed in cultures of purified adult rat RGCs. Importantly, after nerve crush in vivo, we observed a positive effect of OTX2 on the number of regenerating axons up to the optic chiasm within 14 days post crush and a very modest level of acuity absent in control mice. The effect of OTX2 on RGC survival and regeneration is of potential interest for degenerative diseases affecting this cell type. All animal procedures were approved by the local "Comié d'éιthique en expérimentation animale n°59" and authorization n° 00702.01 delivered March 28, 2014 by the French "Ministére de l'enseignement supérieur et de la recherche".

摘要

视网膜神经节细胞(RGC)轴突是光敏感且能进行光子转导的神经视网膜与大脑视觉中枢之间的唯一连接。RGC轴突退化发生在多种致盲疾病中,而刺激存活的神经节细胞进行轴突再生的能力可为视力恢复提供解剖学基础。OTX2是一种在视网膜中表达的同源结构域蛋白转录因子,先前的研究表明,在应激反应中,外源性OTX2可提高RGC在体外和体内的存活率。在此,我们检测并量化了OTX2对成年RGC轴突在体外和体内再生的影响。结果显示,外源性OTX2可刺激成年视网膜细胞解离培养物以及成年视网膜组织外植体中的RGC轴突生长,并且在纯化的成年大鼠RGC培养物中也观察到轴突生长,这表明RGC可直接对外源性OTX2产生反应。重要的是,在体内神经挤压后,我们观察到OTX2对挤压后14天内再生至视交叉的轴突数量有积极影响,并且在对照小鼠中不存在的敏锐度水平也有轻微提升。OTX2对RGC存活和再生的影响对于影响这种细胞类型的退行性疾病具有潜在意义。所有动物实验程序均获得当地“第59号动物实验伦理委员会”的批准,并于2014年3月28日获得法国“高等教育与研究部”颁发的第00702.01号授权。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ca1/8504389/cdbac1deff7a/NRR-17-690-g002.jpg

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