Innate immune receptor signaling induces transient melanoma dedifferentiation while preserving immunogenicity.
Beatrice ThierFang ZhaoSimone StupiaAlicia BrüggemannJohannes KochNina SchulzeSusanne HornChristoph CochGunther HartmannAntje SuckerDirk SchadendorfAnnette PaschenPublished in: Journal for immunotherapy of cancer (2022)
Our results demonstrate that RIG-I signaling in melanoma cells drives a transient phenotypic switch toward a non-proliferative dedifferentiated persister cell state. Despite their dedifferentiation, those persisters are highly immunogenic and sensitive toward autologous TILs, challenging the concept of melanoma dedifferentiation as a general indicator of T cell resistance. In sum, our findings support the application of RIG-I agonists as a therapeutic tool for the generation of long-term clinical benefit in non-resectable melanoma.