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移植表达胰岛素样生长因子-1的人类神经祖细胞可提高视网膜神经节细胞的存活率。

Transplantation of Human Neural Progenitor Cells Expressing IGF-1 Enhances Retinal Ganglion Cell Survival.

作者信息

Ma Jie, Guo Chenying, Guo Caiwei, Sun Yu, Liao Tiffany, Beattie Ursula, López Francisco J, Chen Dong Feng, Lashkari Kameran

机构信息

Schepens Eye Research Institute, Massachusetts Eye and Ear Infirmary, Department of Ophthalmology, Harvard Medical School, Boston, 02114, MA, United States of America.

Ophthalmology DPU, RD. Alternative Discovery & Development, GlaxoSmithKline, King of Prussia, PA, 19406, United States of America.

出版信息

PLoS One. 2015 Apr 29;10(4):e0125695. doi: 10.1371/journal.pone.0125695. eCollection 2015.

Abstract

We have previously characterized human neuronal progenitor cells (hNP) that can adopt a retinal ganglion cell (RGC)-like morphology within the RGC and nerve fiber layers of the retina. In an effort to determine whether hNPs could be used a candidate cells for targeted delivery of neurotrophic factors (NTFs), we evaluated whether hNPs transfected with an vector that expresses IGF-1 in the form of a fusion protein with tdTomato (TD), would increase RGC survival in vitro and confer neuroprotective effects in a mouse model of glaucoma. RGCs co-cultured with hNPIGF-TD cells displayed enhanced survival, and increased neurite extension and branching as compared to hNPTD or untransfected hNP cells. Application of various IGF-1 signaling blockers or IGF-1 receptor antagonists abrogated these effects. In vivo, using a model of glaucoma we showed that IOP elevation led to reductions in retinal RGC count. In this model, evaluation of retinal flatmounts and optic nerve cross sections indicated that only hNPIGF-TD cells effectively reduced RGC death and showed a trend to improve optic nerve axonal loss. RT-PCR analysis of retina lysates over time showed that the neurotrophic effects of IGF-1 were also attributed to down-regulation of inflammatory and to some extent, angiogenic pathways. This study shows that neuronal progenitor cells that hone into the RGC and nerve fiber layers may be used as vehicles for local production and delivery of a desired NTF. Transplantation of hNPIGF-TD cells improves RGC survival in vitro and protects against RGC loss in a rodent model of glaucoma. Our findings have provided experimental evidence and form the basis for applying cell-based strategies for local delivery of NTFs into the retina. Application of cell-based delivery may be extended to other disease conditions beyond glaucoma.

摘要

我们之前已对人神经祖细胞(hNP)进行了表征,该细胞可在视网膜的视网膜神经节细胞(RGC)层和神经纤维层内呈现出类似RGC的形态。为了确定hNP是否可作为神经营养因子(NTF)靶向递送的候选细胞,我们评估了用表达与tdTomato(TD)融合蛋白形式的IGF-1的载体转染的hNP,是否会增加体外RGC的存活率,并在青光眼小鼠模型中发挥神经保护作用。与hNPTD或未转染的hNP细胞相比,与hNPIGF-TD细胞共培养的RGC显示出存活率提高,神经突延伸和分支增加。应用各种IGF-1信号阻断剂或IGF-1受体拮抗剂可消除这些作用。在体内,使用青光眼模型我们发现眼压升高导致视网膜RGC数量减少。在该模型中,对视网膜平铺片和视神经横断面的评估表明,只有hNPIGF-TD细胞有效减少了RGC死亡,并显示出改善视神经轴突损失的趋势。随着时间的推移对视网膜裂解物进行的RT-PCR分析表明,IGF-1的神经营养作用还归因于炎症和在一定程度上血管生成途径的下调。这项研究表明,归巢到RGC层和神经纤维层的神经祖细胞可作为局部产生和递送所需NTF的载体。hNPIGF-TD细胞的移植提高了体外RGC的存活率,并在青光眼啮齿动物模型中防止RGC损失。我们的研究结果提供了实验证据,并为将基于细胞的策略用于向视网膜局部递送NTF奠定了基础。基于细胞的递送应用可能会扩展到青光眼以外的其他疾病情况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b6b/4414591/5a52af6a236c/pone.0125695.g001.jpg

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