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从头发到角膜:毛囊衍生干细胞在治疗角膜缘干细胞缺陷中的治疗用途。

From hair to cornea: toward the therapeutic use of hair follicle-derived stem cells in the treatment of limbal stem cell deficiency.

机构信息

Department of Ophthalmology, University of Erlangen-Nürnberg, Erlangen, Germany.

出版信息

Stem Cells. 2011 Jan;29(1):57-66. doi: 10.1002/stem.550.

Abstract

Limbal stem cell deficiency (LSCD) leads to severe ocular surface abnormalities that can result in the loss of vision. The most successful therapy currently being used is transplantation of limbal epithelial cell sheets cultivated from a limbal biopsy obtained from the patient's healthy, contralateral eye or cadaveric tissue. In this study, we investigated the therapeutic potential of murine vibrissae hair follicle bulge-derived stem cells (HFSCs) as an autologous stem cell (SC) source for ocular surface reconstruction in patients bilaterally affected by LSCD. This study is an expansion of our previously published work showing transdifferentiation of HFSCs into cells of a corneal epithelial phenotype in an in vitro system. In this study, we used a transgenic mouse model, K12(rtTA/rtTA) /tetO-cre/ROSA(mTmG) , which allows for HFSCs to change color, from red to green, once differentiation to corneal epithelial cells occurs and Krt12, the corneal epithelial-specific differentiation marker, is expressed. HFSCs were isolated from transgenic mice, amplified by clonal expansion on a 3T3 feeder layer, and transplanted on a fibrin carrier to the eye of LSCD wild-type mice (n = 31). The HFSC transplant was able to reconstruct the ocular surface in 80% of the transplanted animals; differentiating into cells with a corneal epithelial phenotype, expressing Krt12, and repopulating the corneal SC pool while suppressing vascularization and conjunctival ingrowth. These data highlight the therapeutic properties of using HFSC to treat LSCD in a mouse model while demonstrating a strong translational potential and points to the niche as a key factor for determining stem cell differentiation.

摘要

角膜缘干细胞缺乏症(LSCD)导致严重的眼表面异常,可能导致视力丧失。目前最成功的治疗方法是从患者健康对侧眼或尸体组织中获得的角膜缘活检中培养的角膜缘上皮细胞片进行移植。在这项研究中,我们研究了鼠触须毛囊隆突衍生干细胞(HFSCs)作为自体干细胞(SC)来源用于双侧 LSCD 患者眼表面重建的治疗潜力。这项研究是我们之前发表的工作的扩展,该工作表明 HFSCs 在体外系统中可向角膜上皮表型细胞转化。在这项研究中,我们使用了一种转基因小鼠模型,K12(rtTA/rtTA) /tetO-cre/ROSA(mTmG) ,允许 HFSCs 一旦分化为角膜上皮细胞并表达角膜上皮特异性分化标志物 Krt12,颜色从红色变为绿色。HFSCs 从转基因小鼠中分离出来,在 3T3 饲养层上通过克隆扩增进行扩增,并在纤维蛋白载体上移植到 LSCD 野生型小鼠的眼睛(n = 31)。HFSC 移植能够重建 80%的移植动物的眼表面;分化为具有角膜上皮表型的细胞,表达 Krt12,并重新填充角膜 SC 池,同时抑制血管生成和结膜内长入。这些数据突出了使用 HFSC 治疗 LSCD 的治疗特性在小鼠模型中,同时展示了强大的转化潜力,并指出生态位是决定干细胞分化的关键因素。

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