Identification of Runx1 enhancer element, eR1, that targets tissue stem cells of gastric stem cells
Gastric carcinogenesis is still relatively poorly understood, because of the lack of knowledge of stem cells in stomach.
Yoshiaki Ito, MD PhD
Cancer Science Institute of Singapore, National University of Singapore
Objective: Gastric carcinogenesis is still relatively poorly understood, because of the lack of knowledge of stem cells in stomach. We attempted to molecularly identify gastric stem cells.
Methodology: We reported earlier the 270 bp Runx1 enhancer element that drives the expression of Runx1 in hematopoietic stem cells, termed eR1 (Stem Cells 28:1869-81, 2010). We generated mice harboring eR1-GFP and looked for GFP positive cells. We also generated eR1-CreERT2 mice for lineage tracing as well as for activating oncogenic K-ras.
Results: In stomach, rapidly growing cells are known to be located in the isthmus of both corpus and antrum. We found that GFP+ cells at isthmus of both the corpus and the antrum of mice (Gastroenterology, 2016, PMID27670082). A stem cell marker, Lgr5, was reported to identify stem cells in antrum at the base but never in the isthmus (Cell Stem Cell 6:25-36, 2010). Both Lgr5+ cells and eR1+ cells have the ability to form organoids which are considered to develop only from stem cells. I will discuss about the presence of more than one type of stem cell activities in a given tissue. When oncogenic K-ras was expressed in eR1+ cells, dramatic morphological changes occurred to convert corpus epithelium to become antrum-like epithelium by eliminating parietal cells and chief cells. This phenomenon resembles the antralization observed in chronic gastritis after H pylori infection in human stomach. About 10% of eR1+ cells are also detected in fully differentiated chief cells that express pepsinogen located at the base of corpus. They only rarely proliferate without stress. When oncogenic K-ras is expressed, chief cells can also showed stem cell activity as well as to induce SPEM.
Conclusion: We identified gastric stem cells by eR1 at the predicted location both in corpus and antrum. A subset of chief cells may function as reserve stem cells. Expression of oncogenic K-ras in stem cells induced metaplasia.