Encoding BRAF inhibitor functions in protein degraders.
Daniel S J MillerSabine A VoellGobec Izidor SosičMatic ProjOlivia W RossaneseGregor SchnakenburgMichael GütschowIan CollinsChristian SteinebachPublished in: RSC medicinal chemistry (2022)
Various BRAF kinase inhibitors were developed to treat cancers carrying the BRAF V600E mutation. First-generation BRAF inhibitors could lead to paradoxical activation of the MAPK pathway, limiting their clinical usefulness. Here, we show the development of two series of BRAF V600E -targeting PROTACs and demonstrate that the exchange of the inhibitor scaffold from vemurafenib to paradox-breaker ligands resulted in BRAF V600E degraders that did not cause paradoxical ERK activation.