Randomized Placebo-controlled Analysis of Superior Laryngeal Nerve Block for Neurogenic Cough

Summary

Participation Requirements

Description

Abbreviations/ Definitions: cough severity index (CSI), Cough quality of life questionnaire (CQLQ), proton pump inhibitor (PPI), nasopharyngolaryngoscopy (NPL), University of South Florida (USF), superior laryngeal nerve (SLN), upper airway cough syndrome (UACS), food and drug administration (FDA), ...

Abbreviations/ Definitions: cough severity index (CSI), Cough quality of life questionnaire (CQLQ), proton pump inhibitor (PPI), nasopharyngolaryngoscopy (NPL), University of South Florida (USF), superior laryngeal nerve (SLN), upper airway cough syndrome (UACS), food and drug administration (FDA), investigational new drug (IND), medical record number (MRN), electronic medical record (EMR), ear nose and throat (ENT), angiotensin converting enzyme (ACE), chronic rhinosinusitis (CRS), gastroesophageal reflux disorder (GERD), pulmonary function test (PFT), Reflux finding score (RFS), Speech and language pathology (SLP) Participants will be referred into (via other USF affiliated departments) or recruited within the University of South Florida Department of Otolaryngology practice. Individuals will be screened for eligibility based on referral description. Eligibility will be determined by history at initial visit based on inclusion and exclusion criteria. Eligible participants will be adults with chronic cough >8 weeks duration and presumed neurogenic cough based on initial evaluation. Chronic throat clearing with foreign body sensation for >8 weeks duration will also meet criteria for inclusion and will be used synonymously with and considered chronic cough for the remainder of this protocol and study. Patients will be excluded if primary cause is determined to not be neurogenic. Patients will be excluded if there are other possible significant contributors to the cough that have not been treated (no other obvious treatable and untreated cause), or they will be treated per the standard of care prior to enrolling in this study. Patients will be screened for at least a 4-week course of PPI therapy during duration of symptoms. Patients with possible UACS were included if a trial of medications had been completed previously. If patients are on long term medications that are effective for their respective related condition (but still ineffective at adequately controlling chronic cough), they will be encouraged to make no unnecessary changes through treatment/study duration. These include acid suppression therapy (outside of the recent 6-week trial of PPI if applicable), therapy for UACS symptoms if indicated (eg, Flonase and antihistamine, saline rinses, etc.), neuromodulators (e.g., gabapentin). Patients were excluded if they started any of these medications in last month and were not willing to discontinue them for the duration of the trial. Participants must be willing and able to consent to participate in the study, be willing to be assigned to and undergo intervention or the placebo, and be willing to adhere to the study protocol for the duration of the trial: 2-4 visits, approximately 3 weeks of treatment, 6 week PPI trial with 4 week discontinuation period if no improvement (if applicable), up to 12 week follow up questionnaires (survey only), participate in cough suppression, take PPI as prescribed for duration specified. Participants were excluded if at any point they met the following criteria: unwilling to participate in protocol, allergic to Bupivacaine or triamcinolone acetonide suspension, presence of severe uncontrolled medical condition, any significant pulmonary processes (including chronic obstructive pulmonary disease, bronchiectasis, non-asthmatic eosinophilic bronchitis, structural abnormalities, etc.), presence of asthma (determined by presence of abnormal pulmonary function test (PFT) provocation testing), concern for aerodigestive tract malignancy from history or exam, structural abnormality seen on NPL or prior imaging, immunocompromised, current smoker, use of ACE inhibitor at time of or one month preceding first injection, or vulnerable population. Eligible participants underwent NPL will be also conducted at initial visit (Reflux finding score, RFS). Informed consent will be obtained at this time. Demographics (including sex, age, past medical history, related comorbidities, sidedness of globus sensation, neuromodulator use, results of any prior chest radiograph during symptom duration, ever referred to SLP for voice therapy) will be recorded at initial visit. Related comorbidities include UACS, allergic rhinitis, CRS, GERD. Patients who had not previously received adequate PPI trial were placed in 4 to 6-week course and encourage/counseled to complete lifestyle modifications to reduce reflux. Patients with less than complete response to PPI (persistent clinically significant cough) therapy were included in study. Patients follow-up visit for consideration of injection was schedule one month after discontinuing PPI trial. Questionnaire scores were determined immediately prior to first injection. All patients were counseled on cough suppression prior to initial injection. Patients were randomly assigned to placebo (2-cc normal saline) or intervention (total of 2-cc injection, mixture consisting of 1-cc of Bupivacaine and 1-cc of Kenolog-40) injection groups using computer-generated random assignment. Injections will begin at initial visit or at follow-up visit if trial of PPI required. Immediately preceding injections, patients will be given 5 sprays of 4% topical lidocaine to facilitate injection which will also act to facilitate patient blinding. Injection will be delivered into the region of the proximal superior laryngeal nerve using greater cornu of hyoid and superior cornu of thyroid cartilage as landmarks. Injection will be placed 1-cm anterior to the midpoint of these landmarks. If globus sensation or trigger site was localized to one side, this was recorded and initial injection was directed at this side, otherwise this was picked at random. The second injection was directed at the same side if partial improvement (patient's subjective sense of least 50% reduction of symptoms) was observed after the first injection. The second injection was directed at the contralateral side if there was no initial improvement. Third injection was offered if there was improvement during either of the first two injections (completed on the ipsilateral side of prior two injections or the side with most improvement if bilateral had been completed). There was no second/third injection if complete resolution of symptoms was observed after the preceding injection. Follow up for repeat injection will be scheduled in 1-2 weeks, and exact time recorded. Questionnaire scores were then recorded 2 weeks after final injection of the series. Surveys (see next section, CSI and CQLQ) will also be sent for patients to complete at 6 and 12 weeks after last injection, which will be analyzed in subsequent study. Surveys will have a one-week window to be considered in their nominal category. All adverse events will be recorded. See data capture sheet for collected variables.

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