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牙源性鼻窦炎的炎症表型。

Inflammatory endotype of odontogenic sinusitis.

机构信息

Department of Otolaryngology-Head and Neck Surgery, Henry Ford Health, Detroit, Michigan, USA.

Department of Public Health Sciences, Henry Ford Health, Detroit, Michigan, USA.

出版信息

Int Forum Allergy Rhinol. 2023 Jun;13(6):998-1006. doi: 10.1002/alr.23099. Epub 2022 Nov 8.

Abstract

BACKGROUND

Odontogenic sinusitis (ODS) is distinct from non-odontogenic rhinosinusitis with regard to clinical features as well as diagnostic and therapeutic approaches. While numerous studies have explored immune profiles of chronic rhinosinusitis, very few studies have explored the inflammatory endotype of ODS.

METHODS

Odontogenic sinusitis was diagnosed by confirming infectious sinusitis adjacent to infectious maxillary odontogenic pathology. Maxillary sinus cultures and mucosal biopsies were obtained during endoscopic endonasal surgery in ODS and control patients. Controls were patients undergoing endoscopic skull base surgery with no sinus disease. Specimens were snap frozen in liquid nitrogen and stored at -80°C. Analysis was performed using a multiplex assay to measure Th-1 (TNFα, IFNγ, IL-2,12,18), Th-2 (IL-4,5,9,13), Th-17 (IL-17A,17F,22), and innate (CCL5,CXCL9,CXCL10, IL-6,8,10,12,23,27) immune pathways. Groups were compared via independent sample t-tests; if assumptions were violated, nonparametric Wilcoxon ranked sum tests were performed.

RESULTS

Specimens from 22 ODS patients were compared to nine controls. ODS mucosal tissue was sampled in the setting of the following dental pathologies: post-dental extraction (n = 15), untreated apical periodontitis (n = 2), apical periodontitis after root canal therapy (n = 2), and maxillary sinus bone grafting with or without dental implantation (n = 3). The following cytokines were significantly elevated in ODS compared to controls: IFNγ, TNFα, IL-6, 8, 10, 27, and CXCL9. IL-17 levels were similar in both ODS and controls. Therefore, ODS demonstrated heightened innate and Th1 immune activity.

CONCLUSION

ODS demonstrated both innate immune and Th1 inflammatory endotypes. Further studies are needed to explore ODS immunopathobiology and its potential impact on ODS management.

摘要

背景

牙源性鼻窦炎(ODS)在临床特征以及诊断和治疗方法上与非牙源性鼻-鼻窦炎不同。虽然许多研究已经探索了慢性鼻-鼻窦炎的免疫谱,但很少有研究探索 ODS 的炎症表型。

方法

通过确认感染性上颌牙源性病变相邻的感染性窦炎来诊断牙源性鼻窦炎。在 ODS 和对照组患者的内镜鼻内手术中获取上颌窦培养物和黏膜活检。对照组是接受内镜颅底手术且无窦疾病的患者。标本在液氮中迅速冷冻并储存在-80°C。使用多重分析测定法分析 Th-1(TNFα、IFNγ、IL-2、12、18)、Th-2(IL-4、5、9、13)、Th-17(IL-17A、17F、22)和先天(CCL5、CXCL9、CXCL10、IL-6、8、10、12、23、27)免疫途径。通过独立样本 t 检验比较组间差异;如果违反了假设,则进行非参数 Wilcoxon 秩和检验。

结果

比较了 22 例 ODS 患者和 9 例对照组的标本。ODS 黏膜组织取自以下牙科病变:拔牙后(n=15)、未经治疗的根尖周炎(n=2)、根管治疗后根尖周炎(n=2)和上颌窦骨移植伴或不伴牙种植(n=3)。与对照组相比,ODS 中以下细胞因子显著升高:IFNγ、TNFα、IL-6、8、10、27 和 CXCL9。ODS 和对照组的 IL-17 水平相似。因此,ODS 表现出先天免疫和 Th1 免疫活性增强。

结论

ODS 表现出先天免疫和 Th1 炎症表型。需要进一步研究以探索 ODS 的免疫病理生物学及其对 ODS 管理的潜在影响。

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