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Retinal stem cells transplanted into models of late stages of retinitis pigmentosa preferentially adopt a glial or a retinal ganglion cell fate

机译:视网膜干细胞移植入色素性视网膜炎晚期模型中时,优先采用神经胶质或视网膜神经节细胞命运

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摘要

PURPOSE: To characterize the potential of newborn retinal stem cells (RSCs) isolated from the radial glia population to integrate the retina, this study was conducted to investigate the fate of in vitro expanded RSCs transplanted into retinas devoid of photoreceptors (adult rd1 and old VPP mice and rhodopsin-mutated transgenic mice) or partially degenerated retina (adult VPP mice) retinas. METHODS: Populations of RSCs and progenitor cells were isolated either from DBA2J newborn mice and labeled with the red lipophilic fluorescent dye (PKH26) or from GFP (green fluorescent protein) transgenic mice. After expansion in EGF+FGF2 (epidermal growth factor+fibroblast growth factor), cells were transplanted intravitreally or subretinally into the eyes of adult wild-type, transgenic mice undergoing slow (VPP strain) or rapid (rd1 strain) retinal degeneration. RESULTS: Only limited migration and differentiation of the cells were observed in normal mice injected subretinally or in VPP and rd1 mice injected intravitreally. After subretinal injection in old VPP mice, transplanted cells massively migrated into the ganglion cell layer and, at 1 and 4 weeks after injection, harbored neuronal and glial markers expressed locally, such as beta-tubulin-III, NeuN, Brn3b, or glial fibrillary acidic protein (GFAP), with a marked preference for the glial phenotype. In adult VPP retinas, the grafted cells behaved similarly. Few grafted cells stayed in the degenerating outer nuclear layer (ONL). These cells were, in rare cases, positive for rhodopsin or recoverin, markers specific for photoreceptors and some bipolar cells. CONCLUSIONS: These results show that the grafted cells preferentially integrate into the GCL and IPL and express ganglion cell or glial markers, thus exhibiting migratory and differentiation preferences when injected subretinally. It also appears that the retina, whether partially degenerated or already degenerated, does not provide signals to induce massive differentiation of RSCs into photoreceptors. This observation suggests that a predifferentiation of RSCs into photoreceptors before transplantation may be necessary to obtain graft integration in the ONL.
机译:目的:为表征从放射状胶质细胞群体分离出的新生视网膜干细胞(RSC)整合视网膜的潜力,进行了这项研究以研究将体外扩增的RSC移植到没有光感受器的视网膜中的命运(成人rd1和旧的VPP)小鼠和视紫红质突变的转基因小鼠)或部分变性的视网膜(成人VPP小鼠)视网膜。方法:从DBA2J新生小鼠中分离RSC和祖细胞群,并用红色亲脂性荧光染料(PKH26)或GFP(绿色荧光蛋白)转基因小鼠标记。在EGF + FGF2(表皮生长因子+成纤维细胞生长因子)中扩增后,将细胞玻璃体内或视网膜下移植到经历缓慢(VPP株)或快速(rd1株)视网膜变性的成年野生型转基因小鼠的眼睛中。结果:在视网膜下或VPP中注射的正常小鼠和玻璃体内注射的rd1小鼠仅观察到有限的细胞迁移和分化。在旧的VPP小鼠中进行视网膜下注射后,移植的细胞大量迁移到神经节细胞层中,并且在注射后1和4周,带有局部表达的神经元和神经胶质标志物,例如β-微管蛋白III,NeuN,Brn3b或神经胶质纤维酸性蛋白(GFAP),对神经胶质表型有明显的偏爱。在成年VPP视网膜中,移植细胞的行为类似。很少有移植细胞留在退化的外核层(ONL)中。在极少数情况下,这些细胞对视紫红质或恢复素,感光细胞和某些双极细胞具有特异性的标志物呈阳性。结论:这些结果表明,移植的细胞优先整合到GCL和IPL中并表达神经节细胞或神经胶质标记,因此在视网膜下注射时表现出迁移和分化偏好。看来,视网膜,无论是部分退化还是已经退化,都不能提供诱导RSC大量分化为感光细胞的信号。该观察结果表明,在移植前将RSCs预先分化为感光细胞对于在ONL中获得移植物整合可能是必要的。

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