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生成人类胰岛细胞类型特异性身份基因集。

Generation of human islet cell type-specific identity genesets.

机构信息

Department of Genetic Medicine and Development, Faculty of Medicine, University of Geneva, rue Michel-Servet 1, 1211, Geneva, Switzerland.

Department of Genetics and Evolution, Faculty of Sciences, University of Geneva, Quai Ernest-Ansermet 30, 1211, Geneva, Switzerland.

出版信息

Nat Commun. 2022 Apr 19;13(1):2020. doi: 10.1038/s41467-022-29588-8.

Abstract

Generation of surrogate cells with stable functional identities is crucial for developing cell-based therapies. Efforts to produce insulin-secreting replacement cells to treat diabetes require reliable tools to assess islet cellular identity. Here, we conduct a thorough single-cell transcriptomics meta-analysis to identify robustly expressed markers used to build genesets describing the identity of human α-, β-, γ- and δ-cells. These genesets define islet cellular identities better than previously published genesets. We show their efficacy to outline cell identity changes and unravel some of their underlying genetic mechanisms, whether during embryonic pancreas development or in experimental setups aiming at developing glucose-responsive insulin-secreting cells, such as pluripotent stem-cell differentiation or in adult islet cell reprogramming protocols. These islet cell type-specific genesets represent valuable tools that accurately benchmark gain and loss in islet cell identity traits.

摘要

生成具有稳定功能特征的替代细胞对于开发基于细胞的疗法至关重要。为了生产可分泌胰岛素的替代细胞来治疗糖尿病,需要可靠的工具来评估胰岛细胞的特性。在这里,我们进行了全面的单细胞转录组学元分析,以鉴定用于构建描述人α-、β-、γ-和δ-细胞特性的基因集的稳健表达标记物。这些基因集比以前发表的基因集更能定义胰岛细胞特性。我们展示了它们在勾勒细胞特性变化和揭示一些潜在遗传机制方面的功效,无论是在胚胎胰腺发育过程中,还是在旨在开发葡萄糖反应性胰岛素分泌细胞的实验设置中,如多能干细胞分化或成年胰岛细胞重编程方案。这些胰岛细胞类型特异性基因集是有价值的工具,可以准确地对胰岛细胞特性特征的获得和丧失进行基准测试。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0f3a/9019032/0cfdd131fe79/41467_2022_29588_Fig1_HTML.jpg

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