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Involvement of Laryngopharyngeal Reflux in Select Nonfunctional Laryngeal Diseases: A Systematic Review

期刊

OTOLARYNGOLOGY-HEAD AND NECK SURGERY
卷 164, 期 1, 页码 37-48

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SAGE PUBLICATIONS LTD
DOI: 10.1177/0194599820933209

关键词

reflux; laryngopharyngeal; stenosis; granuloma; vocal folds; infection; laryngeal; tracheal; larynx; leukoplakia

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This study investigated the role of laryngopharyngeal reflux (LPR) in nonfunctional laryngeal diseases and found that the association between LPR and laryngotracheal stenosis, leukoplakia, vocal fold granuloma, and laryngeal papillomatosis is currently not well demonstrated. There is significant heterogeneity among studies regarding inclusion criteria, diagnostic methods, and clinical outcome evaluation. Further clinical and experimental studies are needed to confirm the potential relationship between LPR and these select nonfunctional laryngeal diseases.
Objectives To investigate the existing published evidence supporting the role of laryngopharyngeal reflux (LPR) in the development of the select nonfunctional laryngeal diseases of laryngotracheal stenosis, granuloma, leukoplakia, and laryngeal infections Data Sources PubMed, Cochrane Library, and Scopus. Review Methods A systematic review was performed by 3 independent investigators for studies providing information about the prevalence and role of LPR in the development of laryngotracheal stenosis, granuloma, leukoplakia, and laryngeal infections. Diagnostic criteria and clinical outcome evaluation of included studies were analyzed with PRISMA criteria. Results Of the 64 relevant publications, 27 clinical and 4 basic science studies were included. Ten studies used objective reliable examinations for LPR diagnosis (eg, dual- or triple-probe or oropharyngeal pH monitoring, multichannel intraluminal impedance-pH monitoring, or pepsin detection). According to the bias analysis and the results of studies, the association between LPR and laryngotracheal stenosis, leukoplakia, laryngeal papillomatosis, or vocal fold granuloma remains poorly demonstrated. There is a notable heterogeneity among included studies regarding their inclusion criteria, diagnostic methods, and clinical outcome evaluation. Although some experimental findings support the involvement of bile salts and other gastroduodenal proteins active in alkaline pH, no included clinical studies assessed the role of nonacid and mixed reflux through multichannel intraluminal impedance-pH monitoring. Conclusion The involvement of LPR in the development of leukoplakia, laryngotracheal stenosis, vocal fold granuloma, and laryngeal papillomatosis is currently not demonstrated. The potential relationship between LPR and these select nonfunctional laryngeal diseases must be confirmed through future clinical and experimental studies considering acid, nonacid, and mixed LPR.

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