AI Article Synopsis
- In the MAPK pathway, the V600E mutation in B-Raf kinase leads to constant activation, resulting in excessive activity of downstream kinases MEK and ERK, contributing to melanoma and other cancers.
- Research indicates that existing drugs often fail due to resistance and can paradoxically activate B-Raf; therefore, new drugs targeting allosteric sites are necessary.
- By studying a specific α-helix on B-Raf crucial for its interaction with MEK, the research identifies potential new drug targets to inhibit B-Raf's oncogenic effects in melanoma.
Article Abstract
In the MAPK pathway, an oncogenic V600E mutation in B-Raf kinase causes the enzyme to be constitutively active, leading to aberrantly high phosphorylation levels of its downstream effectors, MEK and ERK kinases. The V600E mutation in B-Raf accounts for more than half of all melanomas and ∼3% of all cancers, and many drugs target the ATP binding site of the enzyme for its inhibition. Because B-Raf can develop resistance against these drugs and such drugs can induce paradoxical activation, drugs that target allosteric sites are needed. To identify other potential drug targets, we generated and kinetically characterized an active form of B-Raf expressed using a bacterial expression system. In doing so, we identified an α-helix on B-Raf, found at the B-Raf-MEK interface, that is critical for their interaction and the oncogenic activity of B-Raf. We assessed the binding between B-Raf mutants and MEK using pull downs and biolayer interferometry and assessed phosphorylation levels of MEK and in cells as well as its downstream target ERK to show that mutating certain residues on this α-helix is detrimental to binding and downstream activity. Our results suggest that this B-Raf α-helix binding site on MEK could be a site to target for drug development to treat B-Raf-induced melanomas.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8407401 | PMC |
| http://dx.doi.org/10.1021/acs.biochem.0c00598 | DOI Listing |
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