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Productive Infection of Human Embryonic Stem Cell-Derived NKX2.1+ Respiratory Progenitors With Human Rhinovirus

机译:人鼻病毒对人胚胎干细胞衍生的NKX2.1 +呼吸祖细胞的生产性感染

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Airway epithelial cells generated from pluripotent stem cells (PSCs) represent a resource for research into a variety of human respiratory conditions, including those resulting from infection with common human pathogens. Using an NKX2.1-GFP reporter human embryonic stem cell line, we developed a serum-free protocol for the generation of NKX2.1+ endoderm that, when transplanted into immunodeficient mice, matured into respiratory cell types identified by expression of CC10, MUC5AC, and surfactant proteins. Gene profiling experiments indicated that day 10 NKX2.1+ endoderm expressed markers indicative of early foregut but lacked genes associated with later stages of respiratory epithelial cell differentiation. Nevertheless, NKX2.1+ endoderm supported the infection and replication of the common respiratory pathogen human rhinovirus HRV1b. Moreover, NKX2.1+ endoderm upregulated expression of IL-6, IL-8, and IL-1B in response to infection, a characteristic of human airway epithelial cells. Our experiments provide proof of principle for the use of PSC-derived respiratory epithelial cells in the study of cell-virus interactions. SignificanceThis report provides proof-of-principle experiments demonstrating, for the first time, that human respiratory progenitor cells derived from stem cells in the laboratory can be productively infected with human rhinovirus, the predominant cause of the common cold.
机译:由多能干细胞(PSC)产生的气道上皮细胞代表了研究各种人类呼吸道疾病的资源,其中包括由普通人类病原体感染引起的疾病。使用NKX2.1-GFP报告基因人类胚胎干细胞系,我们开发了用于生成NKX2.1 +内胚层的无血清方案,当将其移植到免疫缺陷小鼠中时,其成熟度可通过CC10,MUC5AC的表达鉴定为呼吸细胞类型和表面活性剂蛋白质。基因谱分析实验表明,第10天NKX2.1 +内胚层表达的标志物表明了前肠的早期形成,但缺乏与呼吸道上皮细胞分化后期有关的基因。但是,NKX2.1 +内胚层支持常见呼吸道病原体人类鼻病毒HRV1b的感染和复制。此外,NKX2.1 +内胚层响应感染是人气道上皮细胞的特征,上调了IL-6,IL-8和IL-1B的表达。我们的实验提供了使用PSC衍生的呼吸道上皮细胞研究细胞与病毒相互作用的原理证明。重要性本报告提供了原理验证实验,首次证明了实验室中源自干细胞的人呼吸祖细胞可以有效感染人鼻病毒,这是普通感冒的主要原因。

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