<i>BRAF</i> Mutation Correlates With High-Risk Langerhans Cell Histiocytosis and Increased Resistance to First-Line Therapy

Sébastien Héritier(Sorbonne Université), Jean‐François Emile(Sorbonne Université), Mohamed‐Aziz Barkaoui(Sorbonne Université), Caroline Thomas(Sorbonne Université), Sylvie Fraitag(Sorbonne Université), Sabah Boudjemaa(Sorbonne Université), Florence Renaud(Sorbonne Université), Anne Moreau(Sorbonne Université), Michel Peuchmaur(Sorbonne Université), Catherine Chassagne‐Clément(Sorbonne Université), Frédérique Dijoud(Sorbonne Université), Valérie Rigau(Sorbonne Université), Despina Moshous(Sorbonne Université), Anne Lambilliotte(Sorbonne Université), Françoise Mazingue(Sorbonne Université), Kamila Kébaïli(Sorbonne Université), Jean Miron(Sorbonne Université), Éric Jeziorski(Sorbonne Université), Geneviève Plat(Sorbonne Université), Nathalie Aladjidi(Sorbonne Université), Alina Ferster(Sorbonne Université), Hélène Pacquement(Sorbonne Université), Claire Galambrun(Sorbonne Université), Laurence Brugières(Sorbonne Université), Guy Leverger(Sorbonne Université), L Mansuy(Sorbonne Université), Catherine Paillard(Sorbonne Université), Anne Deville(Sorbonne Université), Corinne Armari‐Alla(Sorbonne Université), Anne Lutun(Sorbonne Université), Marion Gillibert‐Yvert(Sorbonne Université), Jean‐Louis Stéphan(Sorbonne Université), Fleur Cohen‐Aubart(Sorbonne Université), Julien Haroche(Sorbonne Université), Isabelle Pellier(Sorbonne Université), Frédéric Millot(Sorbonne Université), Brigitte Lescoeur(Sorbonne Université), Virginie Gandemer(Sorbonne Université), Christine Bodemer(Sorbonne Université), Roger Lacave(Sorbonne Université), Zofia Hélias‐Rodzewicz(Sorbonne Université), Valérie Taly(Sorbonne Université), Frédéric Geissmann(Sorbonne Université), Jean Donadieu(Sorbonne Université)
Journal of Clinical Oncology
July 6, 2016
10.1200/jco.2015.65.9508
Cited by 335Open Access
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Abstract

PURPOSE: Langerhans cell histiocytosis (LCH) is an inflammatory myeloid neoplasia with a broad spectrum of clinical manifestations and outcomes in children. The somatic BRAF(V600E) mutation occurs frequently, but clinical significance remains to be determined. PATIENTS AND METHODS: BRAF(V600E) mutation was investigated in a French LCH cohort. We analyzed associations between mutation status and clinical presentation, extent of disease, reactivation rate, response to therapy, and long-term permanent sequelae. RESULTS: Among 315 patients with successfully determined BRAF status, 173 (54.6%) carried a BRAF(V600E) mutation. Patients with BRAF(V600E) manifested more severe disease than did those with wild-type BRAF. Patients with BRAF(V600E) comprised 87.8% of patients (43 of 49) with multisystem LCH with risk organ involvement (liver, spleen, hematology), 68.6% of patients (35 of 51) with multisystem LCH without risk organ involvement, 43.9% of patients (86 of 196) with single-system LCH, and 42.1% of patients (8 of 19) with lung-involved LCH (P < .001). BRAF(V600E) mutation was also associated with organ involvement that could lead to permanent, irreversible damage, such as neurologic (75%) and pituitary (72.9%) injuries. Compared with patients with wild-type BRAF, patients with BRAF(V600E) more commonly displayed resistance to combined vinblastine and corticosteroid therapy (21.9% v 3.3%; P = .001), showed a higher reactivation rate (5-year reactivation rate, 42.8% v 28.1%; P = .006), and had more permanent, long-term consequences from disease or treatment (27.9% v 12.6%; P = .001). CONCLUSION: In children with LCH, BRAF(V600E) mutation was associated with high-risk features, permanent injury, and poor short-term response to chemotherapy. Further population-based studies should be undertaken to confirm our observations and to assess the impact of BRAF inhibitors for this subgroup of patients who may benefit from targeted therapy.

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