FAT4 loss initiates hepatocarcinogenesis through the switching of canonical to noncanonical WNT signaling pathways

Fung-Yu Huang; Danny Ka-Ho Wong; Lung-Yi Mak; Tan-To Cheung; Sai-Sai Zhang; Hau-Tak Chau; Rex Wan-Hin Hui; Wai-Kay Seto; Man-Fung Yuen

doi:10.1097/HC9.0000000000000338

FAT4 loss initiates hepatocarcinogenesis through the switching of canonical to noncanonical WNT signaling pathways

Hepatol Commun. 2023 Dec 7;7(12):e0338. doi: 10.1097/HC9.0000000000000338. eCollection 2023 Dec 1.

Authors

Fung-Yu Huang¹, Danny Ka-Ho Wong^{1

2}, Lung-Yi Mak^{1

2}, Tan-To Cheung^{2

3}, Sai-Sai Zhang¹, Hau-Tak Chau¹, Rex Wan-Hin Hui¹, Wai-Kay Seto^{1

2}, Man-Fung Yuen^{1

2}

Affiliations

¹ Department of Medicine, School of Clinical Medicine, The University of Hong Kong, Queen Mary Hospital, Hong Kong SAR.
² State Key Laboratory of Liver Research, The University of Hong Kong, Hong Kong SAR.
³ Department of Surgery, School of Clinical Medicine, The University of Hong Kong, Queen Mary Hospital, Hong Kong SAR.

Abstract

Background: Mutation and downregulation of FAT atypical cadherin 4 (FAT4) are frequently detected in HCC, suggesting a tumor suppressor role of FAT4. However, the underlying molecular mechanism remains elusive.

Methods: CRISPR-Cas9 system was used to knockout FAT4 (FAT4-KO) in a normal human hepatic cell line L02 to investigate the impact of FAT4 loss on the development of HCC. RNA-sequencing and xenograft mouse model were used to study gene expression and tumorigenesis, respectively. The mechanistic basis of FAT4 loss on hepatocarcinogenesis was elucidated using in vitro experiments.

Results: We found that FAT4-KO disrupted cell-cell adhesion, induced epithelial-mesenchymal transition, and increased expression of extracellular matrix components. FAT4-KO is sufficient for tumor initiation in a xenograft mouse model. RNA-sequencing of FAT4-KO cells identified PAK6-mediated WNT/β-catenin signaling to promote tumor growth. Suppression of PAK6 led to β-catenin shuttling out of the nucleus for ubiquitin-dependent degradation and constrained tumor growth. Further, RNA-sequencing of amassed FAT4-KO cells identified activation of WNT5A and ROR2. The noncanonical WNT5A/ROR2 signaling has no effect on β-catenin and its target genes (CCND1 and c-Myc) expression. Instead, we observed downregulation of receptors for WNT/β-catenin signaling, suggesting the shifting of β-catenin-dependent to β-catenin-independent pathways as tumor progression depends on its receptor expression. Both PAK6 and WNT5A could induce the expression of extracellular matrix glycoprotein, laminin subunit alpha 4. Laminin subunit alpha 4 upregulation in HCC correlated with poor patient survival.

Conclusions: Our data show that FAT4 loss is sufficient to drive HCC development through the switching of canonical to noncanonical Wingless-type signaling pathways. The findings may provide a mechanistic basis for an in-depth study of the two pathways in the early and late stages of HCC for precise treatment.

MeSH terms

Animals
Cadherins / genetics
Carcinogenesis / genetics
Carcinoma, Hepatocellular* / pathology
Humans
Laminin
Liver Neoplasms* / pathology
Mice
RNA
Tumor Suppressor Proteins / genetics
Tumor Suppressor Proteins / metabolism
Wnt Proteins / genetics
Wnt Signaling Pathway / genetics
beta Catenin / genetics
beta Catenin / metabolism

Substances

beta Catenin
Wnt Proteins
Laminin
RNA
FAT4 protein, human
Cadherins
Tumor Suppressor Proteins