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一种具有残余角膜缘干细胞的角膜缘干细胞缺陷小鼠模型。

A limbal stem cell deficiency murine model with residual limbal stem cells.

作者信息

Someya Hideaki, Shirahama Shintaro, Karg Margarete M, Gregory-Ksander Meredith S, Dana Reza, Ksander Bruce R

出版信息

bioRxiv. 2024 Oct 17:2024.10.17.618942. doi: 10.1101/2024.10.17.618942.

Abstract

Bilateral limbal stem cell deficiency (LSCD) is a significant cause of corneal blindness and is more difficult to treat, as compared with unilateral LSCD because no source of autologous limbal stem cells (LSCs) remains in these patients. Thus, bilateral patients could be candidates for treatment with allogeneic LSC transplants that require long-term systemic immunosuppression therapy. Thus, if possible, for the correct candidates, using autologous LSCs could be a preferred treatment. Recent laser confocal microscopic examination of the ocular surface , combined with impression cytology, has indicated that some patients diagnosed with a complete bilateral LSCD possess residual LSCs. However, it remains unknown whether these residual LSCs still have stem cell potential due to the lack of animal models that mimic this pathology. The goal of the current study is to make a complete LSCD model that possesses evidence of residual LSCs. We induced complete LSCD in mice using two methods: (1) removed the corneal epithelium and the epithelial basement membrane using a rotating burr, and (2) removed the corneal epithelium using 20% ethanol but retained an intact epithelial basement membrane. A complete LSCD was defined by a lack of CK12-positive corneal epithelial cells and the presence of infiltrating CK19-positive conjunctival epithelial cells. Corneas were examined for wound closure, corneal opacity, LSC exhaustion, and inflammation. We observed that complete LSCD mice without an intact epithelial basement membrane resulted in few residual LSCs. By contrast, complete LSCD mice that retained the epithelial basement membrane were accompanied by a reduced inflammatory response plus a significant number of residual LSCs. This model will allow future studies to determine the function of residual LSCs in complete LSCD.

摘要

双侧角膜缘干细胞缺乏(LSCD)是角膜盲的一个重要原因,与单侧LSCD相比更难治疗,因为这些患者没有自体角膜缘干细胞(LSC)来源。因此,双侧患者可能是需要长期全身免疫抑制治疗的同种异体LSC移植的候选者。因此,如果可能的话,对于合适的候选者,使用自体LSC可能是一种首选治疗方法。最近,眼表的激光共聚焦显微镜检查结合印迹细胞学表明,一些被诊断为完全双侧LSCD的患者拥有残余的LSC。然而,由于缺乏模拟这种病理的动物模型,这些残余的LSC是否仍具有干细胞潜能尚不清楚。本研究的目的是建立一个具有残余LSC证据的完全LSCD模型。我们用两种方法在小鼠中诱导完全LSCD:(1)用旋转毛刺去除角膜上皮和上皮基底膜,(2)用20%乙醇去除角膜上皮,但保留完整的上皮基底膜。完全LSCD的定义是缺乏CK12阳性的角膜上皮细胞和存在浸润性CK19阳性的结膜上皮细胞。检查角膜的伤口闭合、角膜混浊、LSC耗竭和炎症情况。我们观察到,没有完整上皮基底膜的完全LSCD小鼠产生的残余LSC很少。相比之下,保留上皮基底膜的完全LSCD小鼠伴有炎症反应减轻和大量残余LSC。该模型将使未来的研究能够确定残余LSC在完全LSCD中的功能。

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A Review of the Diagnosis and Treatment of Limbal Stem Cell Deficiency.角膜缘干细胞缺乏症的诊断与治疗综述
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Prog Retin Eye Res. 2021 Nov;85:100956. doi: 10.1016/j.preteyeres.2021.100956. Epub 2021 Mar 4.

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