功能免疫表型分析鉴定学龄前反复喘息儿童病毒反应的新型内表型。
Functional immunophenotyping of blood neutrophils identifies novel endotypes of viral response in preschool children with recurrent wheezing.
机构信息
Department of Pediatrics, Emory University, Atlanta, Ga; Division of Pulmonary Medicine, Children's Healthcare of Atlanta, Atlanta, Ga.
Department of Pediatrics, Emory University, Atlanta, Ga.
出版信息
J Allergy Clin Immunol. 2023 Dec;152(6):1433-1443. doi: 10.1016/j.jaci.2023.08.010. Epub 2023 Aug 19.
BACKGROUND
Preschool children with recurrent wheezing are heterogeneous, with differing responses to respiratory viral infections. Although neutrophils are crucial for host defense, their function has not been studied in this population.
OBJECTIVE
We performed functional immunophenotyping on isolated blood neutrophils from 52 preschool children with recurrent wheezing (aeroallergen sensitization, n = 16; no sensitization, n = 36).
METHODS
Blood neutrophils were purified and cultured overnight with polyinosinic:polycytidylic acid [poly(I:C)] as a viral analog stimulus. Neutrophils underwent next-generation sequencing with Reactome pathway analysis and were analyzed for cytokine secretion, apoptosis, myeloperoxidase, and extracellular DNA release. CD14 monocytes were also exposed to neutrophil culture supernatant and analyzed for markers of M1 and M2 activation.
RESULTS
A total of 495 genes, related largely to the innate immune system and neutrophil degranulation, were differently expressed in children with versus without aeroallergen sensitization. Functional experiments identified more neutrophil degranulation and extracellular trap formation (ie, more myeloperoxidase and extracellular DNA) and less neutrophil proinflammatory cytokine secretion in children with aeroallergen sensitization. Neutrophils also shifted CD14 monocytes to a more anti-inflammatory (ie, M2) phenotype in sensitized children and a more proinflammatory (ie, M1) phenotype in nonsensitized children. Although both groups experienced viral exacerbations, annualized exacerbation rates prompting unscheduled health care were also higher in children without aeroallergen sensitization after enrollment.
CONCLUSIONS
Systemic neutrophil responses to viral infection differ by allergic phenotype and may be less effective in preschool children without allergic inflammation. Further studies of neutrophil function are needed in this population, which often has less favorable therapeutic responses to inhaled corticosteroids and other therapies directed at type 2-high inflammation.
背景
反复喘息的学龄前儿童存在异质性,对呼吸道病毒感染的反应也不同。尽管中性粒细胞对宿主防御至关重要,但它们在该人群中的功能尚未得到研究。
目的
我们对 52 例反复喘息的学龄前儿童(变应原致敏,n=16;无致敏,n=36)的分离血中性粒细胞进行了功能免疫表型分析。
方法
纯化血液中性粒细胞并与聚肌苷酸:聚胞苷酸(poly[I:C])一起培养过夜作为病毒类似物刺激物。对中性粒细胞进行下一代测序,并进行 Reactome 途径分析,分析细胞因子分泌、凋亡、髓过氧化物酶和细胞外 DNA 释放。还将 CD14 单核细胞暴露于中性粒细胞培养上清液中,并分析 M1 和 M2 激活的标志物。
结果
共有 495 个基因,主要与先天免疫系统和中性粒细胞脱颗粒有关,在有变应原致敏的儿童与无致敏的儿童之间表达不同。功能实验发现,有变应原致敏的儿童中性粒细胞脱颗粒和细胞外陷阱形成(即髓过氧化物酶和细胞外 DNA 增加)更多,促炎细胞因子分泌减少。中性粒细胞还使 CD14 单核细胞向更抗炎(即 M2)表型转变在致敏儿童中,在非致敏儿童中向更促炎(即 M1)表型转变。尽管两组都经历了病毒加重,但在入组后无变应原致敏的儿童中,促使非计划性医疗保健的年度加重率也更高。
结论
对病毒感染的全身中性粒细胞反应因过敏表型而异,在没有过敏炎症的学龄前儿童中可能效果不佳。需要对该人群的中性粒细胞功能进行进一步研究,因为该人群对吸入性皮质类固醇和其他针对 2 型高炎症的治疗的治疗反应往往较差。
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