Supplementary Figure 7 from Genome-Wide Study of Hypomethylated and Induced Genes in Patients with Liver Cancer Unravels Novel Anticancer Targets

Stefanska, Barbara; Cheishvili, David; Suderman, Matthew; Arakelian, Ani; Huang, Jian; Hallett, Michael; Han, Ze-Guang; Al-Mahtab, Mamun; Akbar, Sheikh Mohammad Fazle; Khan, Wasif Ali; Raqib, Rubhana; Tanvir, Imrana; Khan, Haseeb Ahmed; Rabbani, Shafaat A.; Szyf, Moshe

doi:10.1158/1078-0432.22452308.v1

10780432ccr130283-sup-fig7.pdf (689.51 kB)

Supplementary Figure 7 from Genome-Wide Study of Hypomethylated and Induced Genes in Patients with Liver Cancer Unravels Novel Anticancer Targets

journal contribution

posted on 2023-03-31, 17:52 authored by Barbara Stefanska, David Cheishvili, Matthew Suderman, Ani Arakelian, Jian Huang, Michael Hallett, Ze-Guang Han, Mamun Al-Mahtab, Sheikh Mohammad Fazle Akbar, Wasif Ali Khan, Rubhana Raqib, Imrana Tanvir, Haseeb Ahmed Khan, Shafaat A. Rabbani, Moshe Szyf

PDF file - 690KB, Supplementary Figure S7. Impact of RASAL2 and NENF depletion on on expression of genes of DNA methylation machinery, DNMT1, MBD2, DNMT3A, and DNMT3B. DNMT1 (A), MBD2 (B), DNMT3A (C), and DNMT3B (D) expression levels quantified by QPCR in HepG2 and SkHep1 liver cancer cells transfected with siRASAL2 or siNENF as compared to siCtrl. All results represent mean � S.D. of three determinations in either two or three independent experiments - ***P < 0.001, **P < 0.01, *P < 0.05.

History

ARTICLE ABSTRACT

Purpose: We utilized whole-genome mapping of promoters that are activated by DNA hypomethylation in hepatocellular carcinoma (HCC) clinical samples to shortlist novel targets for anticancer therapeutics. We provide a proof of principle of this approach by testing six genes short-listed in our screen for their essential role in cancer growth and invasiveness.Experimental Design: We used siRNA- or shRNA-mediated depletion to determine whether inhibition of these genes would reduce human tumor xenograft growth in mice as well as cell viability, anchorage-independent growth, invasive capacities, and state of activity of nodal signaling pathways in liver, breast, and bladder cancer cell lines.Results: Depletion of EXOSC4, RNMT, SENP6, WBSCR22, RASAL2, and NENF effectively and specifically inhibits cancer cell growth and cell invasive capacities in different types of cancer, but, remarkably, there is no effect on normal cell growth, suggesting a ubiquitous causal role for these genes in driving cancer growth and metastasis. Depletion of RASAL2 and NENF in vitro reduces their growth as explants in vivo in mice. RASAL2 and NENF depletion interferes with AKT, WNT, and MAPK signaling pathways as well as regulation of epigenetic proteins that were previously demonstrated to drive cancer growth and metastasis.Conclusion: Our results prove that genes that are hypomethylated and induced in tumors are candidate targets for anticancer therapeutics in multiple cancer cell types. Because these genes are particularly activated in cancer, they constitute a group of targets for specific pharmacologic inhibitors of cancer and cancer metastasis. Clin Cancer Res; 20(12); 3118–32. ©2014 AACR.