Laryngopharyngeal reflux disease: a pilot study with a new multicomponent.

2026-02
Panminerva medica 67(4)
- Andrea Nacci
- Alberto Galli
- Luca Bastiani
- Silvia Capobianco
- Giorgio Ciprandi

PubMed: 41186604
DOI: 10.23736/s0031-0808.25.05387-x

Study Design

Type: Observational
Population: 22 adult patients (13 females, 9 males; mean age: 49.9 years) with a clinical diagnosis of LPRD
Methods: prospective observational study, treated with the device (one stick twice daily for 2 months) and received standardized behavioral and dietary counseling
Duration: 2 months

Background

This prospective observational study aimed to evaluate the efficacy and safety of a new multicomponent medical device containing Gingigel Pro^®, sodium alginate, Tamarindus indica, hyaluronic acid, and vegetal extracts in patients with laryngopharyngeal reflux disease (LPRD).

Methods

Twenty-two adult patients (13 females, 9 males; mean age: 49.9 years) with a clinical diagnosis of LPRD (R-RSI ≥18 and RSA >14) were enrolled. All patients were treated with the device (one stick twice daily for 2 months) and received standardized behavioral and dietary counseling. Assessments were performed at baseline and after treatment using the Revised Reflux Symptom Index (R-RSI), Voice Handicap Index-10 (VHI-10), and Reflux Sign Assessment (RSA). Patients were stratified into three subgroups based on symptom duration: 0-4 months, 5-8 months, and ≥9 months. Statistical analyses evaluated changes in total and item-specific scores across the overall population and subgroups. Tolerability and adverse events were also recorded.

Results

All outcome scores improved significantly after treatment (P<0.0001 for R-RSI, VHI-10, and RSA). The proportion of patients with pathological R-RSI scores decreased from 100% to 9.1%, and with pathological RSA scores from 100% to 59.1%. Most R-RSI items improved significantly. Specific RSA signs related to acute inflammation (e.g., erythema and edema of the uvula, epiglottis, and vocal folds) also showed significant improvement. No adverse events were reported. Subgroup analysis showed that both symptoms and objective signs improved in all subgroups, with the greatest reductions observed in patients with symptom onset within 0-4 months.

Conclusions

This study provides the first clinical evidence that the tested multicomponent device is effective and safe in improving both subjective symptoms and objective signs of LPRD. The observed greater benefit in patients with recent symptom onset supports early intervention. These findings are consistent with current recommendations that prioritize non-acid-suppressive agents in LPRD management. Further randomized controlled trials are warranted.