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去细胞化的神经视网膜和视网膜色素上皮细胞外基质衍生肽增强了人多能干细胞来源的视网膜类器官中突触标志物的表达和对光的反应性。

Decellularised extracellular matrix-derived peptides from neural retina and retinal pigment epithelium enhance the expression of synaptic markers and light responsiveness of human pluripotent stem cell derived retinal organoids.

机构信息

Institute of Genetic Medicine, Newcastle University, UK.

Institute of Neuroscience, Newcastle University, UK.

出版信息

Biomaterials. 2019 Apr;199:63-75. doi: 10.1016/j.biomaterials.2019.01.028. Epub 2019 Jan 22.

Abstract

Tissue specific extracellular matrices (ECM) provide structural support and enable access to molecular signals and metabolites, which are essential for directing stem cell renewal and differentiation. To mimic this phenomenon in vitro, tissue decellularisation approaches have been developed, resulting in the generation of natural ECM scaffolds that have comparable physical and biochemical properties of the natural tissues and are currently gaining traction in tissue engineering and regenerative therapies due to the ease of standardised production, and constant availability. In this manuscript we report the successful generation of decellularised ECM-derived peptides from neural retina (decel NR) and retinal pigment epithelium (decel RPE), and their impact on differentiation of human pluripotent stem cells (hPSCs) to retinal organoids. We show that culture media supplementation with decel RPE and RPE-conditioned media (CM RPE) significantly increases the generation of rod photoreceptors, whilst addition of decel NR and decel RPE significantly enhances ribbon synapse marker expression and the light responsiveness of retinal organoids. Photoreceptor maturation, formation of correct synapses between retinal cells and recording of robust light responses from hPSC-derived retinal organoids remain unresolved challenges for the field of regenerative medicine. Enhanced rod photoreceptor differentiation, synaptogenesis and light response in response to addition of decellularised matrices from RPE and neural retina as shown herein provide a novel and substantial advance in generation of retinal organoids for drug screening, tissue engineering and regenerative medicine.

摘要

组织特异性细胞外基质 (ECM) 为干细胞的更新和分化提供了结构支持,并使其能够接触到分子信号和代谢物,这些对于指导干细胞的更新和分化是必不可少的。为了在体外模拟这一现象,已经开发出组织脱细胞方法,从而产生了具有天然 ECM 支架的天然组织,由于易于标准化生产和持续供应,目前在组织工程和再生疗法中得到了广泛应用。在本手稿中,我们报告了成功从神经视网膜 (decel NR) 和视网膜色素上皮 (decel RPE) 中生成脱细胞 ECM 衍生肽,并报告了它们对人多能干细胞 (hPSC) 向视网膜类器官分化的影响。我们表明,用 decel RPE 和 RPE 条件培养基 (CM RPE) 补充培养基可显著增加杆状光感受器的生成,而添加 decel NR 和 decel RPE 则可显著增强带状突触标志物的表达和视网膜类器官的光反应性。对于再生医学领域来说,光感受器的成熟、视网膜细胞之间正确突触的形成以及从 hPSC 衍生的视网膜类器官中记录到的稳健光反应仍然是未解决的挑战。如本文所示,添加 RPE 和神经视网膜的脱细胞基质可增强杆状光感受器的分化、突触形成和光反应,为药物筛选、组织工程和再生医学提供了一种新颖而重要的视网膜类器官生成方法。

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