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缺氧提高了从小鼠胚胎干细胞分化而来的光感受器的产量,并改善了体外视网膜发生模型的构建。

Hypoxia increases the yield of photoreceptors differentiating from mouse embryonic stem cells and improves the modeling of retinogenesis in vitro.

机构信息

CABIMER (Centro Andaluz de Biología Molecular y Medicina Regenerativa), Avda. Americo Vespucio s/n, Parque Científico y Tecnológico Cartuja, Sevilla, Spain.

出版信息

Stem Cells. 2013 May;31(5):966-78. doi: 10.1002/stem.1339.

Abstract

Retinitis pigmentosa (RP), a genetically heterogeneous group of diseases together with age-related macular degeneration (AMD), are the leading causes of permanent blindness and are characterized by the progressive dysfunction and death of the light sensing photoreceptors of the retina. Due to the limited regeneration capacity of the mammalian retina, the scientific community has invested significantly in trying to obtain retinal progenitor cells from embryonic stem cells (ESC). These represent an unlimited source of retinal cells, but it has not yet been possible to achieve specific populations, such as photoreceptors, efficiently enough to allow them to be used safely in the future as cell therapy of RP or AMD. In this study, we generated a high yield of photoreceptors from directed differentiation of mouse ESC (mESC) by recapitulating crucial phases of retinal development. We present a new protocol of differentiation, involving hypoxia and taking into account extrinsic and intrinsic cues. These include niche-specific conditions as well as the manipulation of the signaling pathways involved in retinal development. Our results show that hypoxia promotes and improves the differentiation of mESC toward photoreceptors. Different populations of retinal cells are increased in number under the hypoxic conditions applied, such as Crx-positive cells, S-Opsin-positive cells, and double positive cells for Rhodopsin and Recoverin, as shown by immunofluorescence analysis. For the first time, this manuscript reports the high efficiency of differentiation in vivo and the expression of mature rod photoreceptor markers in a large number of differentiated cells, transplanted in the subretinal space of wild-type mice.

摘要

色素性视网膜炎(RP)是一组遗传异质性疾病,与年龄相关性黄斑变性(AMD)一起,是导致永久性失明的主要原因,其特征是视网膜感光细胞的进行性功能障碍和死亡。由于哺乳动物视网膜的再生能力有限,科学界投入了大量精力试图从胚胎干细胞(ESC)中获得视网膜祖细胞。这些细胞代表了视网膜细胞的无限来源,但迄今为止,还没有能够有效地获得特定的细胞群,如感光细胞,使其能够安全地用于未来的 RP 或 AMD 的细胞治疗。在这项研究中,我们通过重现视网膜发育的关键阶段,从定向分化的小鼠 ESC(mESC)中产生了大量的感光细胞。我们提出了一种新的分化方案,涉及缺氧,并考虑了外在和内在的线索。这些包括特定小生境的条件以及对参与视网膜发育的信号通路的操作。我们的结果表明,缺氧促进并改善了 mESC 向感光细胞的分化。在应用的低氧条件下,不同的视网膜细胞群体数量增加,如 Crx 阳性细胞、S-Opsin 阳性细胞和 Rhodopsin 和 Recoverin 双阳性细胞,如免疫荧光分析所示。本文首次报道了在体内高效分化,并在大量分化细胞中表达成熟的杆状光感受器标记物,这些细胞被移植到野生型小鼠的视网膜下腔。

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