![]() Specifically, the adverse effects of hyoscine include dry mouth, dizziness, somnolence, visual impairment, agitation, confusion, and mydriasis ( 9). These therapies carry incomplete efficacy and can have bothersome and dangerous adverse effects, such as drowsiness and dizziness ( 8). Although there is a significant demand for efficacious therapies, the only currently approved treatments in the United States are dimenhydrinate (Dramamine), hyoscine (Scopolamine), and meclizine (Dramamine non-drowsy). Travelers with motion sickness have impaired cognitive performance, which can be of increased burden and danger in professional environments ( 7). The mismatch can occur between two different systems or can be due to mismatch in intra-vestibular sensory inputs (a difference between semicircular canal and otoliths) ( 6). The sensory mismatch resulting in motion sickness has been postulated to be due to discordance between actual and expected movement as perceived by the visual, vestibular, and kinesthetic systems ( 3). The etiology and pathogenesis of disease are most commonly theorized as an aggregation of conflicting sensory information that leads to an unpleasant physiological reaction resulting in the symptoms described above ( 4, 5). Other symptoms may include sweating, dizziness, headache, irritability, loss of appetite, and a cluster of symptoms described as sopite syndrome (yawning, drowsiness, and apathy) ( 3). ![]() Nausea and vomiting are the core symptoms of motion sickness ( 2). ![]() Motion sickness is a disorder that has been plaguing travelers in various vehicles since antiquity ( 1). Across these trips, motion sickness symptoms were significantly lower in the tradipitant group compared to the placebo group (tradipitant = 3.19, placebo = 4.57, p = 0.0235).ĭiscussion: Tradipitant has the potential to be an effective therapy for the prevention of vomiting and treatment of nausea in people with motion sickness. For trips exposed to rough sea conditions, the difference in the incidence of vomiting between the groups was more dramatic (tradipitant = 15.79%, placebo = 72.22%, p = 0.0009). Results: Participants on tradipitant had a significantly lower incidence of vomiting as compared to those on placebo across all boat trips (tradipitant = 17.5%, placebo = 39.7%, p = 0.0039). Severity of motion sickness was assessed with the incidence of vomiting and the MSSS. Participants were randomized 1:1 to tradipitant 170 mg or placebo and completed the Motion Sickness Severity Scale (MSSS) every 30 min, in addition to other assessments. Groups of participants were assigned to one of seven boat trips lasting ~4 h on the Pacific Ocean. Methods: A total of 126 adults participated in the Motion Sifnos study. Here we evaluated the efficacy of tradipitant, a novel NK1 receptor antagonist, in preventing motion sickness in variable sea conditions. Neurokinin-1 (NK1) receptor antagonists have the potential to be effective in improving the symptoms of motion sickness, given the involvement of Substance P in nauseogenic and emetic pathways and the expression of NK1 receptors in the gastrointestinal system. Introduction: Novel therapies are needed for the treatment of motion sickness given the inadequate relief and bothersome and dangerous adverse effects of currently approved therapies.
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