Expanding the clinical spectrum of mosaic BRAF skin phenotypes.

Arthur Sorlin,Virginie Carmignac,Jeanne Amiel,Olivia Boccara,Sylvie Fraitag,Annabel Maruani,Martin Theiler,Lisa Weibel,Yannis Duffourd,Christophe Philippe,Christel Thauvin-Robinet,Laurence Faivre,J-B Rivière,Pierre Vabres,Paul Kuentz

Expanding the clinical spectrum of mosaic BRAF skin phenotypes.

2021

Arthur Sorlin
Virginie Carmignac
Jeanne Amiel
Olivia Boccara
Sylvie Fraitag
Annabel Maruani
Martin Theiler
Lisa Weibel
Yannis Duffourd
Christophe Philippe
Christel Thauvin-Robinet
Laurence Faivre
J-B Rivière
Pierre Vabres
Paul Kuentz

BRAF postzygotic activating mutations have been found in 50% of cases of syringocystadenoma papilliferum (SCAP)1 and in phacomatosis pigmentokeratotica (PPK)2,3 , also possibly caused by HRAS4 mutations. BRAF is a RAS-activating serine/threonine kinase of the MAP kinase pathway, resulting in cell growth and proliferation. BRAF mutations, particularly p.(Val600Glu), are frequently identified in melanoma and other human cancers5 . We report clinical presentations of three patients with postzygotic BRAF mutations in affected skin, identified by next generation sequencing (NGS).

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