TY - JOUR U1 - Zeitschriftenartikel, wissenschaftlich - begutachtet (reviewed) A1 - Schuller, Stefanie A1 - Sieker, Jan A1 - Riemenschneider, Philip A1 - Köhler, Bianca A1 - Drucker, Elisabeth A1 - Weiler, Sofia M. E. A1 - Dauch, Daniel A1 - Sticht, Carsten A1 - Goeppert, Benjamin A1 - Roessler, Stephanie A1 - Ribback, Silvia A1 - Breuhahn, Kai A1 - Fend, Falko A1 - Dombrowski, Frank A1 - Singer, Kerstin A1 - Singer, Stephan ED - Kondylis, Vangelis ED - Heikenwälder, Mathias T1 - HELLS Is Negatively Regulated by Wild-Type P53 in Liver Cancer by a Mechanism Involving P21 and FOXM1 JF - Cancers N2 - Simple Summary The tumor suppressor protein P53 is a major player in preventing liver cancer development and progression. In this study we could show that P53 negatively regulates the expression of Helicase, lymphoid specific (HELLS), previously described as an important pro-tumorigenic epigenetic regulator in hepatocarcinogenesis. The regulatory mechanism included induction of the P53 target gene P21 (CDKN1A) resulting in repression of HELLS via downregulation of the transcription factor Forkhead Box Protein M1 (FOXM1). Our in vitro and in vivo findings indicate an important additional aspect of the tumor suppressive function of P53 in liver cancer linked to epigenetic regulation. Abstract The major tumor suppressor P53 (TP53) acts primarily as a transcription factor by activating or repressing subsets of its numerous target genes, resulting in different cellular outcomes (e.g., cell cycle arrest, apoptosis and senescence). P53-dependent gene regulation is linked to several aspects of chromatin remodeling; however, regulation of chromatin-modifying enzymes by P53 is poorly understood in hepatocarcinogenesis. Herein, we identified Helicase, lymphoid specific (HELLS), a major epigenetic regulator in liver cancer, as a strong and selective P53 repression target within the SNF2-like helicase family. The underlying regulatory mechanism involved P53-dependent induction of P21 (CDKN1A), leading to repression of Forkhead Box Protein M1 (FOXM1) that in turn resulted in downregulation of HELLS expression. Supporting our in vitro data, we found higher expression of HELLS in murine HCCs arising in a Trp53−/− background compared to Trp53+/+ HCCs as well as a strong and highly significant correlation between HELLS and FOXM1 expression in different HCC patient cohorts. Our data suggest that functional or mutational inactivation of P53 substantially contributes to overexpression of HELLS in HCC patients and indicates a previously unstudied aspect of P53′s ability to suppress liver cancer formation. KW - - KW - chromatin remodeling KW - HCC KW - gene repression KW - P53 network UN - https://nbn-resolving.org/urn:nbn:de:gbv:9-opus-59138 SN - 2072-6694 SS - 2072-6694 U6 - https://doi.org/10.3390/cancers14020459 DO - https://doi.org/10.3390/cancers14020459 VL - 14 SP - 20 S1 - 20 PB - MDPI ER -