Spatiotemporal profiling defines persistence and resistance dynamics during targeted treatment of melanoma.
Jill C RubinsteinSergii DomanskyiTodd B SheridanBrian SandersonSungHee ParkJessica KasterHaiyin LiOlga AnczukowMeenhard HerlynJeffrey H ChuangPublished in: bioRxiv : the preprint server for biology (2024)
Tumor evolution is accelerated by application of anti-cancer therapy, resulting in clonal expansions leading to dormancy and subsequently resistance, but the dynamics of this process are incompletely understood. Tracking clonal progression during treatment, we identify conserved, global transcriptional changes and local clone-clone and spatial patterns underlying the emergence of resistance.