Novel germline variant in the histone demethylase and transcription regulator KDM4C induces a multi-cancer phenotype.

The apparent dysregulation of H3K9 trimethylation and KDM4C-associated genes in lymphoblastoid cells supports the hypothesis that the variant is causative of the multi-cancer susceptibility in the family. As the variant is ultrarare, located in the conserved catalytic JmjC domain and predicted pathogenic by the majority of available in silico tools, further studies on the role of in cancer predisposition are warranted.