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单细胞转录组学揭示了人类角膜的异质性,以鉴定新的角膜缘和基质标志物。

Single cell transcriptomics reveals the heterogeneity of the human cornea to identify novel markers of the limbus and stroma.

机构信息

Department of Cell Biology-Inspired Tissue Engineering, MERLN Institute for Technology-Inspired Regenerative Medicine, P.O. Box 616, 6200 MD, Maastricht, The Netherlands.

University Eye Clinic Maastricht, Maastricht University Medical Center+, PO Box 5800, 6202 AZ, Maastricht, The Netherlands.

出版信息

Sci Rep. 2021 Nov 5;11(1):21727. doi: 10.1038/s41598-021-01015-w.

Abstract

The cornea is the clear window that lets light into the eye. It is composed of five layers: epithelium, Bowman's layer, stroma, Descemet's membrane and endothelium. The maintenance of its structure and transparency are determined by the functions of the different cell types populating each layer. Attempts to regenerate corneal tissue and understand disease conditions requires knowledge of how cell profiles vary across this heterogeneous tissue. We performed a single cell transcriptomic profiling of 19,472 cells isolated from eight healthy donor corneas. Our analysis delineates the heterogeneity of the corneal layers by identifying cell populations and revealing cell states that contribute in preserving corneal homeostasis. We identified expression of CAV1, HOMER3 and CPVL in the corneal epithelial limbal stem cell niche, CKS2, STMN1 and UBE2C were exclusively expressed in highly proliferative transit amplifying cells, CXCL14 was expressed exclusively in the suprabasal/superficial limbus, and NNMT was exclusively expressed by stromal keratocytes. Overall, this research provides a basis to improve current primary cell expansion protocols, for future profiling of corneal disease states, to help guide pluripotent stem cells into different corneal lineages, and to understand how engineered substrates affect corneal cells to improve regenerative therapies.

摘要

角膜是让光线进入眼睛的透明窗口。它由五层组成:上皮、鲍曼层、基质、德斯梅特膜和内皮。其结构和透明度的维持取决于每层中不同细胞类型的功能。为了再生角膜组织和了解疾病状况,需要了解细胞形态如何在这种异质组织中变化。我们对 8 位健康供体角膜中分离的 19472 个细胞进行了单细胞转录组谱分析。我们的分析通过鉴定细胞群体并揭示有助于维持角膜内稳态的细胞状态,描绘了角膜各层的异质性。我们在角膜上皮缘干细胞龛中鉴定到了 CAV1、HOMER3 和 CPVL 的表达,CKS2、STMN1 和 UBE2C 仅在高度增殖的过渡扩增细胞中表达,CXCL14 仅在基底/浅层角膜缘中表达,而 NNMT 仅由基质成纤维细胞表达。总的来说,这项研究为改进当前的原代细胞扩增方案提供了基础,有助于对角膜疾病状态进行未来的分析,有助于指导多能干细胞向不同的角膜谱系分化,并了解工程化基质如何影响角膜细胞以改善再生疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5814/8571304/9296a133e76f/41598_2021_1015_Fig1_HTML.jpg

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