SUV420H2 is an epigenetic regulator of epithelial/mesenchymal states in pancreatic cancer

Author:

Viotti Manuel1,Wilson Catherine1,McCleland Mark1,Koeppen Hartmut1ORCID,Haley Benjamin1ORCID,Jhunjhunwala Suchit1,Klijn Christiaan1ORCID,Modrusan Zora1,Arnott David1,Classon Marie1,Stephan Jean-Philippe1,Mellman Ira1ORCID

Affiliation:

1. Genentech, South San Francisco, CA

Abstract

Epithelial-to-mesenchymal transition is implicated in metastasis, where carcinoma cells lose sessile epithelial traits and acquire mesenchymal migratory potential. The mesenchymal state is also associated with cancer stem cells and resistance to chemotherapy. It might therefore be therapeutically beneficial to promote epithelial identity in cancer. Because large-scale cell identity shifts are often orchestrated on an epigenetic level, we screened for candidate epigenetic factors and identified the histone methyltransferase SUV420H2 (KMT5C) as favoring the mesenchymal identity in pancreatic cancer cell lines. Through its repressive mark H4K20me3, SUV420H2 silences several key drivers of the epithelial state. Its knockdown elicited mesenchymal-to-epithelial transition on a molecular and functional level, and cells displayed decreased stemness and increased drug sensitivity. An analysis of human pancreatic cancer biopsies was concordant with these findings, because high levels of SUV420H2 correlated with a loss of epithelial characteristics in progressively invasive cancer. Together, these data indicate that SUV420H2 is an upstream epigenetic regulator of epithelial/mesenchymal state control.

Funder

Genentech

Publisher

Rockefeller University Press

Subject

Cell Biology

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