Pediatric retrograde cricopharyngeal dysfunction diagnosed by high‐resolution impedance manometry

Author:

Dorfman Lev1ORCID,El‐Chammas Khalil12,Mansi Sherief12,Graham Kahleb12,Kaul Ajay12

Affiliation:

1. Division of Gastroenterology, Hepatology and Nutrition Cincinnati Children's Hospital Medical Center Cincinnati Ohio USA

2. Department of Pediatrics University of Cincinnati College of Medicine Cincinnati Ohio USA

Abstract

AbstractObjectivesThe inability to burp, known as retrograde cricopharyngeal dysfunction (R‐CPD), was initially described in adults. The proposed clinical diagnostic criteria for R‐CPD include belching inability, abdominal bloating and discomfort/nausea, postprandial chest pain, and involuntary noises. Botulinum toxin injection to the cricopharyngeal muscle has been reported to be beneficial. High‐resolution esophageal impedance‐manometry (HRIM) features in adolescent patients with R‐CPD have not been described yet.  The aim of our study was to describe the clinical and HRIM findings of pediatric patients with R‐CPD.MethodsClinical and manometric features of five pediatric patients diagnosed with R‐CPD were reviewed. HRIM study protocol was modified to include the consumption of carbonated drink to provoke symptoms and distinctive manometric features.ResultsWe report five female patients aged 15–20 years who presented with an inability to burp and involuntary throat sounds. HRIM revealed normal upper esophageal sphincter (UES) relaxation during swallowing, but abnormal UES relaxation with concurrent high esophageal impedance reflecting air entrapment and secondary peristalsis following the carbonated drink challenge. Four patients exhibited esophageal motility disorder. All patients reported improvement or resolution of symptoms after botulinum toxin injection to the cricopharyngeus muscle.ConclusionsAdolescents with an inability to burp, reflux‐like symptoms, bloating, and involuntary throat noises should be assessed for R‐CPD by pediatric gastroenterologists with HRIM. The relatively recent recognition of this novel condition is the likely reason for its under‐ and misdiagnosis in children.

Publisher

Wiley

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