Novel BRAF mutation in melanoma: A case report

Abstract: Abstract. In melanoma, a number of specific genetic and genomic aberrations have been identified to be important in tumorigenesis. In particular, the mutant B-Raf proto-oncogene, Serine/Threonine kinase (BRAF) gene is the target of tailored therapy with kinase inhibitor molecules. Identification of the array of mutations in patients with melanoma will be useful in determining a genetic profile of the tumor with potential implications for treatment decisions. A rare aminoacidic insertion in codon 599 of the BRA… Show more

“…Approximately 30-72% of melanomas have been associated with a BRAF mutation in the V600 codon [4,5]. Most BRAF mutations occur as a missense mutation of a valine replaced by a glutamic acid at codon V600E in exon 15, which lies within the activation segment of the kinase domain disrupting the auto-inhibitory mechanism, resulting in the constitutive activation of the MAPK pathway and facilitating the acquisition of secondary genetic events in tumorigenesis [6,7].…”

<b><i>BRAF</i></b> V600 Mutational Status in Melanoma Correlates with Cytologic Features in Fine-Needle Aspirate Specimens

“…Approximately 30-72% of melanomas have been associated with a BRAF mutation in the V600 codon [4,5]. Most BRAF mutations occur as a missense mutation of a valine replaced by a glutamic acid at codon V600E in exon 15, which lies within the activation segment of the kinase domain disrupting the auto-inhibitory mechanism, resulting in the constitutive activation of the MAPK pathway and facilitating the acquisition of secondary genetic events in tumorigenesis [6,7].…”

<b><i>BRAF</i></b> V600 Mutational Status in Melanoma Correlates with Cytologic Features in Fine-Needle Aspirate Specimens

“…The mutation consists of a heterozygous in‐frame three‐base‐pair insertion at position 1796 (c.1796_1797insCAC), resulting in the insertion of an additional threonine residue at amino‐acid position 599 (p.T599_V600insT), equivalent to the mutation described in the COSMIC database . This mutation was previously found in some cases of thyroid carcinoma and in one patient with metastatic melanoma who died before BRAFi treatment could be started . In silico and in vitro data indicate that rare and/or complex mutations in codons 599–601 increase kinase activity similar to the typical V600E mutation .…”

“…4 This mutation was previously found in some cases of thyroid carcinoma and in one patient with metastatic melanoma who died before BRAFi treatment could be started. 5 In silico and in vitro data indicate that rare and/or complex mutations in codons 599-601 increase kinase activity similar to the typical V600E mutation. 5 In our case, partial remission occurred within 6 weeks, which suggests that combined treatment with BRAFi and MEKi is a valuable treatment option.…”

A rare BRAF T599dup mutation conferring sensitivity to BRAF inhibitor in a patient with metastatic melanoma

“…This mutation was reported in melanomas and melanocytic nevi, leading to activation of RAS/RAF/MEK/ERK pathway, a key player in the initiation of melanocytic tumors [ 7 , 8 ]. A novel BRAF mutation (an aminoacidic insertion in codon 599) was identified in a melanoma patient in the P-loop activating site, mutation that was not discovered before in melanoma, but was detected rarely in Papillary Thyroid Carcinoma and Anaplastic Thyroid Carcinoma, which highlights the heterogeneity of this disease [ 54 ].…”

“…In addition, regulates negatively RAS family leading to RAF inhibitor resistance. To note, NF1 mutations or suppression might appear in parallel to BRAF mutations [ 51 , 52 , 53 , 54 ].…”

Cutaneous Melanoma—A Long Road from Experimental Models to Clinical Outcome: A Review