Targeting G9a/DNMT1 methyltransferase activity impedes IGF2-mediated survival in hepatoblastoma

Salih Demir; Negin Razizadeh; Emilie Indersie; Sophie Branchereau; Stefano Cairo; Roland Kappler

doi:10.1097/HC9.0000000000000378

Targeting G9a/DNMT1 methyltransferase activity impedes IGF2-mediated survival in hepatoblastoma

Hepatol Commun. 2024 Jan 29;8(2):e0378. doi: 10.1097/HC9.0000000000000378. eCollection 2024 Feb 1.

Authors

Salih Demir¹, Negin Razizadeh¹, Emilie Indersie², Sophie Branchereau³, Stefano Cairo^{2

4}, Roland Kappler¹

Affiliations

¹ Department of Pediatric Surgery, Dr. von Hauner Children's Hospital, LMU University Hospital, LMU Munich, Germany.
² XenTech, Evry, France.
³ Department of Pediatric Surgery, Bicêtre Hospital, AP-HP Paris Saclay University, France.
⁴ Champions Oncology, Inc., Rockville, Maryland, USA.

Abstract

Background: As the variable clinical outcome of patients with hepatoblastoma (HB) cannot be explained by genetics alone, the identification of drugs with the potential to effectively reverse epigenetic alterations is a promising approach to overcome poor therapy response. The gene ubiquitin like with PHD and ring finger domains 1 (UHRF1) represents an encouraging epigenetic target due to its regulatory function in both DNA methylation and histone modifications and its clinical relevance in HB.

Methods: Patient-derived xenograft in vitro and in vivo models were used to study drug response. The mechanistic basis of CM-272 treatment was elucidated using RNA sequencing and western blot experiments.

Results: We validated in comprehensive data sets that UHRF1 is highly expressed in HB and associated with poor outcomes. The simultaneous pharmacological targeting of UHRF1-dependent DNA methylation and histone H3 methylation by the dual inhibitor CM-272 identified a selective impact on HB patient-derived xenograft cell viability while leaving healthy fibroblasts unaffected. RNA sequencing revealed downregulation of the IGF2-activated survival pathway as the main mode of action of CM-272 treatment, subsequently leading to loss of proliferation, hindered colony formation capability, reduced spheroid growth, decreased migration potential, and ultimately, induction of apoptosis in HB cells. Importantly, drug response depended on the level of IGF2 expression, and combination assays showed a strong synergistic effect of CM-272 with cisplatin. Preclinical testing of CM-272 in a transplanted patient-derived xenograft model proved its efficacy but also uncovered side effects presumably caused by its strong antitumor effect in IGF2-driven tumors.

Conclusions: The inhibition of UHRF1-associated epigenetic traces, such as IGF2-mediated survival, is an attractive approach to treat high-risk HB, especially when combined with the standard-of-care therapeutic cisplatin.

MeSH terms

CCAAT-Enhancer-Binding Proteins / genetics
CCAAT-Enhancer-Binding Proteins / metabolism
Cisplatin / pharmacology
DNA (Cytosine-5-)-Methyltransferase 1 / antagonists & inhibitors
Hepatoblastoma* / drug therapy
Hepatoblastoma* / genetics
Histone-Lysine N-Methyltransferase / antagonists & inhibitors
Humans
Insulin-Like Growth Factor II / genetics
Insulin-Like Growth Factor II / metabolism
Liver Neoplasms* / drug therapy
Liver Neoplasms* / genetics
Ubiquitin-Protein Ligases / genetics

Substances

CCAAT-Enhancer-Binding Proteins
Cisplatin
IGF2 protein, human
Insulin-Like Growth Factor II
Ubiquitin-Protein Ligases
UHRF1 protein, human
EHMT2 protein, human
DNMT1 protein, human
DNA (Cytosine-5-)-Methyltransferase 1
Histone-Lysine N-Methyltransferase