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人成年纤维状角膜缘干细胞体外生成胰腺内分泌细胞。

In vitro generation of pancreatic endocrine cells from human adult fibroblast-like limbal stem cells.

机构信息

Sezione di Endocrinologia, Dipartimento Biomedico di Medicina Interna e Specialistica, Università degli Studi di Palermo, Palermo, Italy.

出版信息

Cell Transplant. 2012;21(1):73-90. doi: 10.3727/096368911X580635. Epub 2011 Jun 9.

Abstract

Stem cells might provide unlimited supply of transplantable cells for β-cell replacement therapy in diabetes. The human limbus is a highly specialized region hosting a well-recognized population of epithelial stem cells, which sustain the continuous renewal of the cornea, and the recently identified stromal fibroblast-like stem cells (f-LSCs), with apparent broader plasticity. However, the lack of specific molecular markers for the identification of the multipotent limbal subpopulation has so far limited the investigation of their differentiation potential. In this study we show that the human limbus contains uncommitted cells that could be potentially harnessed for the treatment of diabetes. Fourteen limbal biopsies were obtained from patients undergoing surgery for ocular diseases not involving the conjunctiva or corneal surface. We identified a subpopulation of f-LSCs characterized by robust proliferative capacity, expressing several pluripotent stem cell markers and exhibiting self-renewal ability. We then demonstrated the potential of f-LSCs to differentiate in vitro into functional insulin-secreting cells by developing a four-step differentiation protocol that efficiently directed f-LSCs towards the pancreatic endocrine cell fate. The expression of specific endodermal, pancreatic, islet, and β-cell markers, as well as functional properties of f-LSC-derived insulin-producing cells, were evaluated during differentiation. With our stage-specific approach, up to 77% of f-LSCs eventually differentiated into cells expressing insulin (also assessed as C-peptide) and exhibited phenotypic features of mature β-cells, such as expression of critical transcription factors and presence of secretory granules. Although insulin content was about 160-fold lower than what observed in adult islets, differentiated cells processed ∼98% of their proinsulin content, similar to mature β-cells. Moreover, they responded in vitro in a regulated manner to multiple secretory stimuli, including glucose. In conclusion, f-LSCs represent a possible relevant source of autologous, transplantable, insulin-producing cells that could be tested for the reversal of diabetes.

摘要

干细胞可能为糖尿病的β细胞替代治疗提供无限供应的可移植细胞。人角膜缘是一个高度特化的区域,拥有公认的上皮干细胞群,这些细胞维持着角膜的持续更新,以及最近发现的基质成纤维细胞样干细胞(f-LSCs),具有明显更广泛的可塑性。然而,缺乏用于鉴定多能性角膜缘亚群的特定分子标记物,迄今为止限制了对其分化潜能的研究。在这项研究中,我们表明人角膜缘包含未分化的细胞,这些细胞可能被用于治疗糖尿病。从因眼部疾病而接受手术的患者中获得了 14 个角膜缘活检样本,这些疾病不涉及结膜或角膜表面。我们鉴定出一种 f-LSCs 亚群,其具有强大的增殖能力,表达多种多能干细胞标记物,并具有自我更新能力。然后,我们通过开发一种四步分化方案,证明了 f-LSCs 在体外分化为功能性胰岛素分泌细胞的潜力,该方案有效地将 f-LSCs 引导到胰腺内分泌细胞命运。在分化过程中,评估了 f-LSC 衍生的胰岛素产生细胞的特定内胚层、胰腺、胰岛和β细胞标记物的表达以及功能特性。使用我们的阶段特异性方法,多达 77%的 f-LSCs 最终分化为表达胰岛素(也评估为 C 肽)的细胞,并表现出成熟β细胞的表型特征,例如关键转录因子的表达和分泌颗粒的存在。尽管胰岛素含量比成年胰岛中观察到的低 160 倍,但分化细胞处理了其前胰岛素含量的约 98%,类似于成熟β细胞。此外,它们在体外以调节方式对多种分泌刺激物(包括葡萄糖)做出反应。总之,f-LSCs 代表了一种可能的相关自体、可移植、产生胰岛素的细胞来源,可用于测试逆转糖尿病。

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