Ring1b-dependent epigenetic remodelling is an essential prerequisite for pancreatic carcinogenesis.

Benitz, Simone; Straub, Tobias; Mahajan, Ujjwal Mukund; Mutter, Jurik; Czemmel, Stefan; Unruh, Tatjana; Wingerath, Britta; Deubler, Sabrina; Fahr, Lisa; Cheng, Tao; Nahnsen, Sven; Bruns, Philipp; Kong, Bo; Raulefs, Susanne; Ceyhan, Güralp O; Mayerle, Julia; Steiger, Katja; Esposito, Irene; Kleeff, Jörg; Michalski, Christoph W; Regel, Ivonne

doi:10.1136/gutjnl-2018-317208

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Title:: Ring1b-dependent epigenetic remodelling is an essential prerequisite for pancreatic carcinogenesis.
Document type:: Journal Article
Author(s):: Benitz, Simone; Straub, Tobias; Mahajan, Ujjwal Mukund; Mutter, Jurik; Czemmel, Stefan; Unruh, Tatjana; Wingerath, Britta; Deubler, Sabrina; Fahr, Lisa; Cheng, Tao; Nahnsen, Sven; Bruns, Philipp; Kong, Bo; Raulefs, Susanne; Ceyhan, Güralp O; Mayerle, Julia; Steiger, Katja; Esposito, Irene; Kleeff, Jörg; Michalski, Christoph W; Regel, Ivonne
Abstract:: BACKGROUND AND AIMS: Besides well-defined genetic alterations, the dedifferentiation of mature acinar cells is an important prerequisite for pancreatic carcinogenesis. Acinar-specific genes controlling cell homeostasis are extensively downregulated during cancer development; however, the underlying mechanisms are poorly understood. Now, we devised a novel in vitro strategy to determine genome-wide dynamics in the epigenetic landscape in pancreatic carcinogenesis. DESIGN: With our in vitro carcinogenic sequence, we performed global gene expression analysis and ChIP sequencing for the histone modifications H3K4me3, H3K27me3 and H2AK119ub. Followed by a comprehensive bioinformatic approach, we captured gene clusters with extensive epigenetic and transcriptional remodelling. Relevance of Ring1b-catalysed H2AK119ub in acinar cell reprogramming was studied in an inducible Ring1b knockout mouse model. CRISPR/Cas9-mediated Ring1b ablation as well as drug-induced Ring1b inhibition were functionally characterised in pancreatic cancer cells. RESULTS: The epigenome is vigorously modified during pancreatic carcinogenesis, defining cellular identity. Particularly, regulatory acinar cell transcription factors are epigenetically silenced by the Ring1b-catalysed histone modification H2AK119ub in acinar-to-ductal metaplasia and pancreatic cancer cells. Ring1b knockout mice showed greatly impaired acinar cell dedifferentiation and pancreatic tumour formation due to a retained expression of acinar differentiation genes. Depletion or drug-induced inhibition of Ring1b promoted tumour cell reprogramming towards a less aggressive phenotype. CONCLUSIONS: Our data provide substantial evidence that the epigenetic silencing of acinar cell fate genes is a mandatory event in the development and progression of pancreatic cancer. Targeting the epigenetic repressor Ring1b could offer new therapeutic options. «
BACKGROUND AND AIMS: Besides well-defined genetic alterations, the dedifferentiation of mature acinar cells is an important prerequisite for pancreatic carcinogenesis. Acinar-specific genes controlling cell homeostasis are extensively downregulated during cancer development; however, the underlying mechanisms are poorly understood. Now, we devised a novel in vitro strategy to determine genome-wide dynamics in the epigenetic landscape in pancreatic carcinogenesis. DESIGN: With our in vitro carci... »
Journal title abbreviation:: Gut
Year:: 2019
Journal volume:: 68
Journal issue:: 11
Pages contribution:: 2007-2018
Fulltext / DOI:: doi:10.1136/gutjnl-2018-317208
Pubmed ID:: http://view.ncbi.nlm.nih.gov/pubmed/30954952
Print-ISSN:: 0017-5749
TUM Institution:: Chirurgische Klinik und Poliklinik; Institut für Allgemeine Pathologie und Pathologische Anatomie
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