Single cell transcriptome analysis defines heterogeneity of the murine pancreatic ductal tree

Author:

Hendley Audrey Marie1,Rao Arjun Arkal1,Leonhardt Laura1,Ashe Sudipta1,Smith Jennifer A1,Giacometti Simone1,Peng Xianlu L1,Jiang Honglin1,Berrios David1,Pawlak Mathias2,Li Lucia Y1,Lee Jonghyun1,Collisson Eric A1ORCID,Anderson Mark S1ORCID,Fragiadakis Gabriela K1,Yeh Jen Jen3,Chun Jimmie Ye1,Kim Grace E1,Weaver Valerie M1,Hebrok Matthias1ORCID

Affiliation:

1. University of California, San Francisco, San Francisco, United States

2. N/A, BlueRock Therapeutics, Boston, United States

3. University of North Carolina Chapel Hill, Chapel Hill, United States

Abstract

To study disease development, an inventory of an organ's cell types and understanding of physiologic function is paramount. Here, we performed single-cell RNA sequencing to examine heterogeneity of murine pancreatic duct cells, pancreatobiliary cells, and intrapancreatic bile duct cells. We describe an epithelial-mesenchymal transitory axis in our three pancreatic duct subpopulations and identify osteopontin as a regulator of this fate decision as well as human duct cell dedifferentiation. Our results further identify functional heterogeneity within pancreatic duct subpopulations by elucidating a role for geminin in accumulation of DNA damage in the setting of chronic pancreatitis. Our findings implicate diverse functional roles for subpopulations of pancreatic duct cells in maintenance of duct cell identity and disease progression and establish a comprehensive road map of murine pancreatic duct cell, pancreatobiliary cell, and intrapancreatic bile duct cell homeostasis.

Funder

National Cancer Institute

Hirshberg Foundation for Pancreatic Cancer Research

Parker Institute for Cancer Immunotherapy

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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