The mouse HP1 proteins are not required for cell viability but are essential for preventing liver tumorigenesis

Chromatin organization plays essential roles in cell identity and functions. Here, we demonstrated by hepatocyte-specific inactivation of the genes encoding the three Heterochromatin Protein 1 (HP1α, β and γ) in mice (HP1-TKO) that these proteins are dispensable for hepatocyte activity and survival. Conversely, the chronic absence of these proteins led to a drastic increased incidence of liver tumor development. Molecular characterization of HP1-TKO hepatocytes revealed that HP1 proteins are required for maintenance of histone marks associated with heterochromatin, and for the appropriate expression of large number of genes involved in liver-specific functions as well as in genes encoding for transcriptional repressors of the KRAB-ZFP family. Moreover, several specific endogenous retrovirus families were upregulated in HP1-TKO hepatocytes, leading to the deregulated expression of genes in their vicinity. Our findings indicate that HP1 proteins act as guardians of liver homeostasis to prevent tumor development through the modulation of multiple chromatin-associated events.