Purpose: Understanding the function of BRAF mutants is crucial for determining the best treatment strategy. This study aimed to characterize a rare variant, , which was identified in a patient with lung adenocarcinoma (LUAD) by comprehensive genomic profiling.
Materials And Methods: We report a case of LUAD with treated with dabrafenib and trametinib. We conditionally expressed wild-type BRAF, BRAF, or BRAF in Ba/F3 cells and BEAS-2B cells. Ba/F3 cells carrying double-mutant BRAF (BRAF, BRAF, or BRAF) that lacked the dimerizing ability were also established. Knockout of endogenous or in Ba/F3-BRAF cells and Ba/F3-BRAF cells was performed using the CRISPR/Cas9 system. Cell viability, mitogen-activated protein kinase (MAPK) signaling activity, and sensitivity to dabrafenib and trametinib were evaluated.
Results: The patient was revealed to have -positive tumor cells as a predominant clone, and dabrafenib and trametinib treatment showed modest efficacy. In Ba/F3 cells, both BRAF and BRAF similarly caused interleukin-3-independent proliferation and activated the MAPK pathway. Moreover, BRAF and BRAF similarly caused a significant increase in the anchorage-independent growth ability of BEAS-2B cells. Along with Ba/F3-BRAF cells, Ba/F3-BRAF cells were highly sensitive to a monomer-specific BRAF inhibitor, dabrafenib, with a half-maximal inhibitory concentration value of 29.7 nM. In the absence of wild-type BRAF, wild-type CRAF, or an intact dimer interface, the ability to induce oncogenic addiction and MAPK pathway activation in Ba/F3-BRAF cells was not affected, which was in contrast to the findings in the BRAF double-mutant model.
Conclusion: is a potent driver oncogene that activates the MAPK pathway without the requirement for dimerization in vitro. Because has been recurrently reported across various cancer types, our findings should be further investigated both mechanistically and clinically.
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