BACKGROUND: Langerhans cell histiocytosis (LCH) is a disease that arises from myeloid cells that phenotypically resemble Langerhans cells (LC), which is typically driven by the BRAF V600E mutation. High-risk LCH has a poor prognosis. PROCEDURE: Fifteen children with BRAF V600E + LCH received vemurafenib between March 2016 and February 2020. The median age at LCH onset was 2 months and the median age at the start of vemurafenib treatment was 22 months. The median disease activity score (DAS) at the start of vemurafenib treatment was 12 points. RESULTS: The median duration of vemurafenib treatment was 29 months. All patients responded to treatment, with median DAS of 4 points at week 4 and 1 point at 6 months. Two patients died: 1 of hepatic failure after NSAID overdose and 1 of neutropenic sepsis. Cessation of vemurafenib resulted in relapse in 5 patients and was only possible for 1 patient. Serial measurements of BRAF V600E using cell-free circulating DNA revealed that 7 patients had persistently high mutant allele levels. CONCLUSION: Vemurafenib is effective in children with BRAF V600E + LCH. However, treatment with vemurafenib does not eradicate the disease and its long-term toxicity has not been established.
BACKGROUND: Langerhans cell histiocytosis (LCH) is a disease that arises from myeloid cells that phenotypically resemble Langerhans cells (LC), which is typically driven by the BRAF V600E mutation. High-risk LCH has a poor prognosis. PROCEDURE: Fifteen children with BRAF V600E + LCH received vemurafenib between March 2016 and February 2020. The median age at LCH onset was 2 months and the median age at the start of vemurafenib treatment was 22 months. The median disease activity score (DAS) at the start of vemurafenib treatment was 12 points. RESULTS: The median duration of vemurafenib treatment was 29 months. All patients responded to treatment, with median DAS of 4 points at week 4 and 1 point at 6 months. Two patients died: 1 of hepatic failure after NSAID overdose and 1 of neutropenic sepsis. Cessation of vemurafenib resulted in relapse in 5 patients and was only possible for 1 patient. Serial measurements of BRAF V600E using cell-free circulating DNA revealed that 7 patients had persistently high mutant allele levels. CONCLUSION: Vemurafenib is effective in children with BRAF V600E + LCH. However, treatment with vemurafenib does not eradicate the disease and its long-term toxicity has not been established.
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Authors: Jean Donadieu; Islam Amine Larabi; Mathilde Tardieu; Johannes Visser; Caroline Hutter; Elena Sieni; Nabil Kabbara; Mohamed Barkaoui; Jean Miron; François Chalard; Paul Milne; Julien Haroche; Fleur Cohen; Zofia Hélias-Rodzewicz; Nicolas Simon; Mathilde Jehanne; Alexandra Kolenova; Anne Pagnier; Nathalie Aladjidi; Pascale Schneider; Geneviève Plat; Anne Lutun; Anne Sonntagbauer; Thomas Lehrnbecher; Alina Ferster; Viktoria Efremova; Martina Ahlmann; Laurence Blanc; James Nicholson; Anne Lambilliote; Houda Boudiaf; Andrej Lissat; Karel Svojgr; Fanette Bernard; Sarah Elitzur; Michal Golan; Dmitriy Evseev; Michael Maschan; Ahmed Idbaih; Olga Slater; Milen Minkov; Valerie Taly; Matthew Collin; Jean-Claude Alvarez; Jean-François Emile; Sébastien Héritier Journal: J Clin Oncol Date: 2019-09-12 Impact factor: 44.544