Effect of Laryngopharyngeal Reflux and Potassium‐Competitive Acid Blocker (P‐CAB) on the Microbiological Comprise of the Laryngopharynx

Abstract

AbstractObjectiveTo probe the microbiota composition progressing from healthy individuals to those with laryngopharyngeal reflux disease (LPRD) and subsequently undergoing potassium‐competitive acid inhibitor (P‐CAB) therapy.Study DesignProspective case‐control study.SettingAcademic Medical Center.MethodsForty patients with LPRD and 51 patients without LPRD were recruited. An 8‐week P‐CAB therapy was initiated (post‐T‐LPRD), and 39 had return visits. In total, 130 laryngopharyngeal saliva samples were collected and sequenced by targeting the V3‐V4 region of the 16S ribosomal RNA (rRNA) gene using an Illumina MiSeq. Amplicon sequence variants (ASVs) and clinical indices were analyzed.ResultsAlpha and beta diversities were compared among the non‐LPRD, LPRD, and post‐T‐LPRD groups, and the Observed_ASVs were not significantly different. At the same time, the Shannon and Simpson indices, unweighted Unifrac, weighted Unifrac, and binary Jaccard distance were significantly different between non‐LPRD and LPRD groups. In addition, significant differences were found in the abundance of Streptococcus, Prevotella, and Prevotellaceae in the LPRD versus non‐LPRD groups, and Neisseria, Leptotrichia, and Allprevotella in the LPRD versus post‐T‐LPRD groups. The genera model was used to distinguish patients with LPRD from those without, and a better receiver operating characteristic curve was formed after combining the clinical indices of reflux symptom index, reflux finding score, and pepsin, with an area under the curve of 0.960.ConclusionLaryngopharyngeal microbial communities changed after laryngopharyngeal reflux and were modified further after P‐CAB treatment, which provides a potential diagnostic value for LPRD, especially when combined with clinical indices.