Commitment and oncogene-induced plasticity of human stem cell-derived pancreatic acinar and ductal organoids
Ling Huang, Ridhdhi Desai, Daniel N. Conrad, Nayara C. Leite, Dipikaa Akshinthala, Christine Lim, Raul S. González, Lakshmi Muthuswamy, Zev J. Gartner, Senthil K. Muthuswamy
Abstract
The exocrine pancreas, consisting of ducts and acini, is the site of origin of pancreatitis and pancreatic ductal adenocarcinoma (PDAC). Our understanding of the genesis and progression of human pancreatic diseases, including PDAC, is limited because of challenges in maintaining human acinar and ductal cells in culture. Here we report induction of human pluripotent stem cells toward pancreatic ductal and acinar organoids that recapitulate properties of the neonatal exocrine pancreas. Expression of the PDAC-associated oncogene GNAS R201C induces cystic growth more effectively in ductal than acinar organoids, whereas KRAS G12D is more effective in modeling cancer in vivo when expressed in acinar compared with ductal organoids. KRAS G12D , but not GNAS R201C , induces acinar-to-ductal metaplasia-like changes in culture and in vivo . We develop a renewable source of ductal and acinar organoids for modeling exocrine development and diseases and demonstrate lineage tropism and plasticity for oncogene action in the human pancreas.