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原发性纤毛运动障碍的气道细胞对生物膜形成的易感性增加。

Primary ciliary dyskinesia ciliated airway cells show increased susceptibility to biofilm formation.

机构信息

Primary Ciliary Dyskinesia Centre, University Hospital Southampton NHS Foundation Trust, Southampton, UK.

NIHR Southampton Biomedical Research Centre, University of Southampton and University Hospital Southampton NHS Foundation Trust, Southampton, UK.

出版信息

Eur Respir J. 2017 Sep 10;50(3). doi: 10.1183/13993003.00612-2017. Print 2017 Sep.

Abstract

Non-typeable (NTHi) is the most common pathogen in primary ciliary dyskinesia (PCD) patients. We hypothesised that abnormal ciliary motility and low airway nitric oxide (NO) levels on airway epithelial cells from PCD patients might be permissive for NTHi colonisation and biofilm development.We used a primary epithelial cell co-culture model to investigate NTHi infection. Primary airway epithelial cells from PCD and non-PCD patients were differentiated to ciliation using an air-liquid interface culture and then co-cultured with NTHi.NTHi adherence was greater on PCD epithelial cells compared to non-PCD cells (p<0.05) and the distribution of NTHi on PCD epithelium showed more aggregated NTHi in biofilms (p<0.001). Apart from defective ciliary motility, PCD cells did not significantly differ from non-PCD epithelial cells in the degree of ciliation and epithelial integrity or in cytokine, LL-37 and NO production. Treatment of PCD epithelia using exogenous NO and antibiotic significantly reduced NTHi viability in biofilms compared with antibiotic treatment alone.Impaired ciliary function was the primary defect in PCD airway epithelium underlying susceptibility to NTHi biofilm development compared with non-PCD epithelium. Although NO responses were similar, use of targeted NO with antibiotics enhanced killing of NTHi in biofilms, suggesting a novel therapeutic approach.

摘要

无法分型流感嗜血杆菌(NTHi)是原发性纤毛运动障碍(PCD)患者中最常见的病原体。我们假设PCD 患者气道上皮细胞的纤毛运动异常和气道一氧化氮(NO)水平低可能有利于 NTHi 定植和生物膜的形成。我们使用原代上皮细胞共培养模型来研究 NTHi 感染。使用空气-液体界面培养将 PCD 和非 PCD 患者的原代气道上皮细胞分化为纤毛细胞,然后与 NTHi 共培养。与非 PCD 细胞相比,NTHi 在 PCD 上皮细胞上的黏附性更强(p<0.05),NTHi 在 PCD 上皮上的分布显示生物膜中聚集更多的 NTHi(p<0.001)。除了纤毛运动缺陷外,PCD 细胞在纤毛形成程度、上皮完整性或细胞因子、LL-37 和 NO 产生方面与非 PCD 上皮细胞没有显著差异。与单独使用抗生素相比,用外源性 NO 和抗生素处理 PCD 上皮可显著降低生物膜中 NTHi 的活力。与非 PCD 上皮相比,PCD 气道上皮中纤毛功能受损是其对 NTHi 生物膜形成易感性的主要缺陷。尽管 NO 反应相似,但使用靶向 NO 与抗生素联合使用可增强生物膜中 NTHi 的杀伤作用,提示一种新的治疗方法。

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