作者
Jason Gotlib,Mariana Castells,Hanneke Oude Elberink,Frank Siebenhaar,Karin Hartmann,Sigurd Broesby‐Olsen,Tracy I. George,Jens Panse,Iván Álvarez-Twöse,Deepti Radia,Tsewang Tashi,C. Bulaï Livideanu,Vito Sabato,Mark L. Heaney,Paul Van Daele,Sonia Cerquozzi,Ingunn Dybedal,Andreas Reiter,Thanai Pongdee,Stéphane Barète,Celalettin Üstün,Lawrence B. Schwartz,Brant R. Ward,Philippe Schafhausen,Peter Vadas,Prithviraj Bose,Daniel J. DeAngelo,Lindsay Rein,Pankit Vachhani,Massimo Triggiani,Patrizia Bonadonna,Mark Rafferty,Nauman M. Butt,Stephen T. Oh,Friederike Wortmann,Johanna Ungerstedt,Mar Guilarte,Minakshi Taparia,Andrew Kuykendall,Cecilia Arana Yi,Princess Ogbogu,C. Gaudy‐Marqueste,Mattias Mattsson,William Shomali,Matthew P. Giannetti,Ilda Bidollari,Huimin Lin,Erin Sulllivan,Brenton G. Mar,Robyn M. Scherber,Maria Roche,Cem Akin,Marcus Maurer
摘要
BackgroundIndolent systemic mastocytosis (ISM) is a clonal mast-cell disease driven by the KIT D816V mutation. We assessed the efficacy and safety of avapritinib versus placebo, both with best supportive care, in patients with ISM. MethodsWe randomized patients with moderate to severe ISM (total symptom score [TSS] of ≥28; scores range from 0 to 110, with higher numbers indicating more severe symptoms) two to one to avapritinib 25 mg once daily (n=141) or placebo (n=71). The primary end point was mean change in TSS based on the 14-day average of patient-reported severity of 11 symptoms. Secondary end points included reductions in serum tryptase and blood KIT D816V variant allele fraction (≥50%), reductions in TSS (≥50% and ≥30%), reduction in bone marrow mast cells (≥50%), and quality of life measures. ResultsFrom baseline to week 24, avapritinib-treated patients had a decrease of 15.6 points (95% CI, −18.6 to −12.6) in TSS compared to a decrease of 9.2 points (−13.1 to −5.2) in the placebo group; P<0.003. From baseline to Week 24, 76/141 patients (54%; 45% to 62%) in the avapritinib group compared to 0/71 patients in the placebo group achieved a ≥50% reduction in serum tryptase level; P<0.001. Edema and increases in alkaline phosphatase were more common with avapritinib than placebo; there were few treatment discontinuations because of adverse events. ConclusionsIn this trial, avapritinib was superior to placebo in reducing uncontrolled symptoms and mast-cell burden in patients with ISM. The long-term safety and efficacy of this approach for patients with ISM remain the focus of the ongoing trial. (Funded by Blueprint Medicines Corporation; ClinicalTrials.gov number, NCT03731260.)