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    BIOMARKER:

    BRAF G466V

    i
    Other names: BRAF, B-raf proto-oncogene, B-raf proto-oncogene, Serine/threonine kinase, V-Raf murine sarcoma viral oncogene homolog B, Serine/threonine-protein kinase B-Raf, Proto-oncogene B-Raf, BRAF1, RAFB1, B-raf proto-oncogene Serine/threonine-protein kinase, Murine sarcoma viral (V-Raf) oncogene homolog B1, B-raf serine/threonine-protein, 94 KDa B-raf protein, B-RAF1
    Entrez ID:
    673
    Related biomarkers:
    Expression
    Mutation
    CNA
    Fusion
    Others
    almost2years
    Primary mediastinal seminoma with leiomyosarcoma: a rare case report. (PubMed, Cell Mol Biol (Noisy-le-grand))
    Finally, our study demonstrated that the patient benefited from the treatment of chemotherapy alone, or combined with target therapy after the operation. Meanwhile, the BRAF p.G466V, TP53 mutations, MTOR p.T1977I and exons 2-5 deletion of FLCN may be potential molecular mechanisms and oncogenic drivers of this disease.
    Journal
    |
    BRAF (B-raf proto-oncogene) • TP53 (Tumor protein P53) • mTOR (Mechanistic target of rapamycin kinase) • FLCN (Folliculin)
    |
    TP53 mutation • BRAF mutation • MTOR mutation • BRAF G466V
    2years
    Preclinical evaluation of CFT1946 as a selective degrader of mutant BRAF for the treatment of BRAF driven cancers (AACR 2022)
    BRAF inhibitors including vemurafenib, dabrafenib and encorafenib have produced impressive responses in V600X patients, however resistance usually emerges within a year, including RAS mutation, BRAFV600E amplification, and BRAFV600E intragenic deletion or splice variants...The combination of encorafenib and trametinib showed no activity in the same model...Based on its activity in preclinical models, including models of BRAF inhibitor resistance, and its drug-like properties we are progressing CFT1946 as a candidate for clinical development in patients with solid tumors bearing BRAF V600X mutations. Further, given CFT1946’s activity on non-V600 BRAF mutations, we are continuing to explore CFT1946 and related BiDAC degraders as therapeutic options for patients bearing Class II or Class III BRAF mutations.
    Preclinical
    |
    KRAS (KRAS proto-oncogene GTPase) • BRAF (B-raf proto-oncogene) • CRBN (Cereblon)
    |
    BRAF V600E • KRAS mutation • BRAF mutation • NRAS mutation • NRAS Q61 • BRAF G466V • BRAF G469A
    |
    Mekinist (trametinib) • Zelboraf (vemurafenib) • Tafinlar (dabrafenib) • Braftovi (encorafenib) • CFT1946
    over2years
    [VIRTUAL] Lung Cancer Diagnosis in Absence of Adequate Tissue Molecular Analysis in Metastatic Disease by NGS Analysis of Plasma cfDNA (IASLC-WCLC 2021)
    17 TP53 p.R249S 18 TP53 p.R158H 19 TP53 p.S215R 20 TP53 p.P278L 21 TP53 p.R283H 22 TP53 p.P278S; TP53 p.G279E; TP53 c.375+3_375+4insG; p.? 23 TP53 p.R267Q 24 TP53 p.C238F; TP53 p.C275S 25 TP53 p.Y163C 26 TP53 p.R248W 27 TP53 p.S241F 28 TP53 p.V272G Conclusion For patients in whom molecular analysis on tissue cannot be performed, NGS analysis of cfDNA in plasma provides an opportunity to detect driver mutations for subsequent targeted therapy.
    Next-generation sequencing
    |
    EGFR (Epidermal growth factor receptor) • KRAS (KRAS proto-oncogene GTPase) • BRAF (B-raf proto-oncogene) • TP53 (Tumor protein P53) • PIK3CA (Phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha)
    |
    TP53 mutation • KRAS G12C • BRAF mutation • PIK3CA mutation • EGFR exon 19 deletion • KRAS G12D • EGFR exon 20 insertion • KRAS G12V • PIK3CA E545K • KRAS G12 • KRAS Q61H • BRAF G466V • PIK3CA E545 • EGFR E746 • KRAS V12
    |
    CELLSEARCH® • Oncomine™ Lung cfDNA Assay
    almost3years
    [VIRTUAL] The landscape of BRAF alteration in Chinese solid tumor patients (ESMO 2021)
    Vemurafenib and dabrafenib have already been approved for the treatment of melanoma, NSCLC and colorectal carcinoma. BRAF gene mutations, especially BRAF non-V600, was extensively mutated in Chinese multiple cancer types. Our revealed the potential targeted therapeutic strategies among non-V600 population with solid tumors should be considered in further study.
    Clinical • BRCA Biomarker
    |
    EGFR (Epidermal growth factor receptor) • KRAS (KRAS proto-oncogene GTPase) • BRAF (B-raf proto-oncogene) • ALK (Anaplastic lymphoma kinase) • TP53 (Tumor protein P53) • PIK3CA (Phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha) • BRCA2 (Breast cancer 2, early onset) • PTEN (Phosphatase and tensin homolog)
    |
    TP53 mutation • BRAF V600E • KRAS mutation • PIK3CA mutation • PTEN mutation • BRAF fusion • BRAF K601E • BRAF D594G • BRAF G466V • BRAF G469A • BRAF D594N • BRAF T599 • BRAF K601
    |
    Zelboraf (vemurafenib) • Tafinlar (dabrafenib)
    almost3years
    NGS-based liquid-biopsy profiling identifies mechanisms of resistance to ALK inhibitors: a step towards personalized NSCLC treatment. (PubMed, Mol Oncol)
    Finally, a c-MYC gain, along with a loss of CCND1 and FGFR3, were detected in a patient progressing on a first-line treatment with crizotinib. We conclude that NGS analysis of liquid biopsies upon disease progression identified different putative ALK-I-resistance mutations in most cases, and could be a valuable approach for therapy decision making.
    Journal • Liquid biopsy • Next-generation sequencing
    |
    EGFR (Epidermal growth factor receptor) • BRAF (B-raf proto-oncogene) • ALK (Anaplastic lymphoma kinase) • TP53 (Tumor protein P53) • PIK3CA (Phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha) • FGFR2 (Fibroblast growth factor receptor 2) • MYC (V-myc avian myelocytomatosis viral oncogene homolog) • IDH2 (Isocitrate Dehydrogenase (NADP(+)) 2) • FGFR3 (Fibroblast growth factor receptor 3) • MAP2K1 (Mitogen-activated protein kinase kinase 1) • CCND1 (Cyclin D1) • SMAD4 (SMAD family member 4) • CCND3 (Cyclin D3)
    |
    TP53 mutation • EGFR mutation • BRAF mutation • PIK3CA mutation • EGFR exon 19 deletion • ALK positive • FGFR2 mutation • ALK mutation • MAP2K1 mutation • ALK G1202R • ALK G1269A • BRAF G466V • MAP2K1 F129L
    |
    Xalkori (crizotinib)
    over3years
    The first small molecules capable of strongly suppressing proliferation of cancer cells harboring BRAF class I/II/III mutations. (PubMed, Biochem Biophys Res Commun)
    In addition, GNF-7 and SIJ1227 suppress more strongly migration/invasion of these cancer cells than vemurafenib and PLX8394. Taken together, both GNF-7 and SIJ1227 are much superior to vemurafenib and PLX8394 in terms of capability to inhibit all classes of BRAF mutants.
    Journal
    |
    BRAF (B-raf proto-oncogene)
    |
    BRAF V600E • BRAF mutation • BRAF V600 • BRAF G466V • BRAF G469A
    |
    Zelboraf (vemurafenib) • plixorafenib (FORE-8394)
    almost4years
    [VIRTUAL] The clinical effect of concurrent oncogenic gene mutations in BRAF p.(V600E)-mutated NSCLC treated with dabrafenib and trametinib (ESMO 2020)
    Legal entity responsible for the study: The authors. Funding: Has not received any funding.
    Clinical
    |
    BRAF (B-raf proto-oncogene) • PIK3CA (Phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha) • IDH1 (Isocitrate dehydrogenase (NADP(+)) 1) • AKT1 (V-akt murine thymoma viral oncogene homolog 1) • GNAS (GNAS Complex Locus)
    |
    BRAF V600E • PIK3CA mutation • BRAF V600 • PIK3CA H1047R • IDH1 R132C • BRAF G466V • BRAF G466V + KIT K509Q • GNAS R201C • PIK3CA G1049R + AKT1 E17K • BRAF K601
    |
    Mekinist (trametinib) • Tafinlar (dabrafenib)