Unknown,Transcriptomics,Genomics,Proteomics

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RNA-seq of purified human pancreatic dedifferentiated acinar cells and duct cells


ABSTRACT: Pancreatic acinar cells can dedifferentiate upon tissue injury and acquire ductal characteristics. This acquisition of duct cell features is critical in tumor development. Nevertheless, duct cells themselves are less prone for development of PDAC (pancreatic ductal adenocarcinoma) than dedifferentiated acini. We aimed to clarify which genes are unique for dedifferentiated acini. Mixed exocrine preparations of acinar and duct cells were obtained from human pancreatic donor organs and cultured to induce dedifferentiation. We lineage-labeled and FACS-purified these human dedifferentiated acinar cells and compared them to duct cells from the same donor (n=5).

INSTRUMENT(S): NextSeq 500

ORGANISM(S): Homo sapiens

SUBMITTER: Ilse Rooman 

PROVIDER: E-MTAB-9386 | biostudies-arrayexpress |

REPOSITORIES: biostudies-arrayexpress

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Publications

MECOM permits pancreatic acinar cell dedifferentiation avoiding cell death under stress conditions.

Backx Elyne E   Wauters Elke E   Baldan Jonathan J   Van Bulck Mathias M   Michiels Ellis E   Heremans Yves Y   De Paep Diedert Luc DL   Kurokawa Mineo M   Goyama Susumu S   Bouwens Luc L   Jacquemin Patrick P   Houbracken Isabelle I   Rooman Ilse I  

Cell death and differentiation 20210324 9


Maintenance of the pancreatic acinar cell phenotype suppresses tumor formation. Hence, repetitive acute or chronic pancreatitis, stress conditions in which the acinar cells dedifferentiate, predispose for cancer formation in the pancreas. Dedifferentiated acinar cells acquire a large panel of duct cell-specific markers. However, it remains unclear to what extent dedifferentiated acini differ from native duct cells and which genes are uniquely regulating acinar cell dedifferentiation. Moreover, m  ...[more]

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