Germline mutation in BRAF codon 600 is compatible with human development: de novo p.V600G mutation identified in a patient with CFC syndrome |
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| Authors: | KJ Champion C Bunag AL Estep JR Jones CH Bolt RC Rogers KA Rauen DB Everman |
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| Institution: | 1. Greenwood Genetic Center, Greenwood, SC, USA;2. Department of Pediatrics, University of California, San Francisco, CA, USA;3. UCSF Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, CA, USA |
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| Abstract: | Champion KJ, Bunag C, Estep AL, Jones JR, Bolt CH, Rogers RC, Rauen KA, Everman DB. Germline mutation in BRAF codon 600 is compatible with human development: de novo p.V600G mutation identified in a patient with CFC syndrome. BRAF, the protein product of BRAF, is a serine/threonine protein kinase and one of the direct downstream effectors of Ras. Somatic mutations in BRAF occur in numerous human cancers, whereas germline BRAF mutations cause cardio‐facio‐cutaneous (CFC) syndrome. One recurrent somatic mutation, p.V600E, is frequently found in several tumor types, such as melanoma, papillary thyroid carcinoma, colon cancer, and ovarian cancer. However, a germline mutation affecting codon 600 has never been described. Here, we present a patient with CFC syndrome and a de novo germline mutation involving codon 600 of BRAF, thus providing the first evidence that a pathogenic germline mutation involving this critical codon is not only compatible with development but can also cause the CFC phenotype. In vitro functional analysis shows that this mutation, which replaces a valine with a glycine at codon 600 (p.V600G), leads to increased ERK and ELK phosphorylation compared to wild‐type BRAF but is less strongly activating than the cancer‐associated p.V600E mutation. |
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| Keywords: | BRAF cardio‐facio‐cutaneous syndrome germline Ras/MAPK pathway RASopathy signal transduction p V600E p V600G |
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