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Rhinovirus C targets ciliated airway epithelial cells

机译:鼻病毒C靶向纤毛气道上皮细胞

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BackgroundThe Rhinovirus C (RV-C), first identified in 2006, produce high symptom burdens in children and asthmatics, however, their primary target host cell in the airways remains unknown. Our primary hypotheses were that RV-C target ciliated airway epithelial cells (AECs), and that cell specificity is determined by restricted and high expression of the only known RV-C cell-entry factor, cadherin related family member 3 (CDHR3). MethodsRV-C15 (C15) infection in differentiated human bronchial epithelial cell (HBEC) cultures was assessed using immunofluorescent and time-lapse epifluorescent imaging. Morphology of C15-infected differentiated AECs was assessed by immunohistochemistry. ResultsC15 produced a scattered pattern of infection, and infected cells were shed from the epithelium. The percentage of cells infected with C15 varied from 1.4 to 14.7% depending on cell culture conditions. Infected cells had increased staining for markers of ciliated cells (acetylated-alpha-tubulin [aat], p p =?ns). CDHR3 expression was increased on ciliated epithelial cells, but not other epithelial cells ( p p ConclusionsThe RV-C only replicate in ciliated AECs in vitro, leading to infected cell shedding. CDHR3 expression positively correlates with RV-C binding and replication, and is largely confined to ciliated AECs. Our data imply that factors regulating differentiation and CDHR3 production may be important determinants of RV-C illness severity.
机译:背景鼻病毒C(RV-C)于2006年首次发现,在儿童和哮喘患者中产生较高的症状负担,但是,它们在呼吸道中的主要靶宿主细胞仍然未知。我们的主要假设是RV-C靶向纤毛气道上皮细胞(AEC),而细胞特异性是由唯一已知的RV-C细胞进入因子钙粘着蛋白相关家族成员3(CDHR3)的限制性表达和高表达决定的。方法采用免疫荧光和延时荧光成像技术评估分化的人支气管上皮细胞(HBEC)培养中的RV-C15(C15)感染。通过免疫组织化学评估C15感染的分化的AEC的形态。结果C15产生了分散的感染模式,并且感染的细胞从上皮脱落。取决于细胞培养条件,被C15感染的细胞百分比在1.4%至14.7%之间变化。感染的细胞对纤毛细胞标记物的染色增加(乙酰化的α-微管蛋白[aat],p p =Δns)。结论:纤毛上皮细胞中CDHR3的表达增加,而其他上皮细胞中CDHR3的表达却没有增加(第pp结论)RV-C仅在纤毛AEC中体外复制,导致感染的细胞脱落。我们的数据表明调节分化和CDHR3产生的因素可能是决定RV-C疾病严重程度的重要因素。

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