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Poster display session

178P - Chief cell in stomach have stem cell activity and potential to develop gastric cancer

Date

23 Nov 2019

Session

Poster display session

Topics

Tumour Site

Gastric Cancer

Presenters

Akihiro Yamamura

Citation

Annals of Oncology (2019) 30 (suppl_9): ix42-ix67. 10.1093/annonc/mdz422

Authors

A. Yamamura1, J. Matsuo2, M. Lim Yi Hui2, D. Liana Heng2, K. Kofu2, Z.H. Md2, D. Douchi2, K.G. Yeoh3, T. Kamei1, T. Naitoh1, M. Osato2, M. Unno1, Y. Ito2

Author affiliations

  • 1 Department Of Surgery, Tohoku University Graduate School of Medicine, 980-8574 - Sendai/JP
  • 2 Cancer Science Institute Of Singapore, National University of Singapore, 117599 - Singapore/SG
  • 3 Gastroenterology And Hepatology, National University Health System, 119228 - Singapore/SG

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Abstract 178P

Background

Rapidly proliferating stomach stem cells have been predicted to be located at the isthmus of both corpus and antrum. We recently identified such stem cells by using 270 bp Runx1 enhancer element, eR1 (Gastroenterol, 2017). In addition, eR1 also marked small number of fully differentiated chief cells in the corpus. We investigated whether chief cells have stem cell activity and can be an origin of gastric cancer, particularly because there are disagreements among the researchers.

Methods

We generated knock-in mice of pepsinogen C-CreERT2 and crossed them with Rosa26-EYFP mice or pepsinogen A-CreERT2 and crossed them with Rosa26-tdTomato mice for lineage tracing. PGC-CreERT2 mice were also crossed with K-rasG12D/+, Trp53flox/flox and Apcflox/floxmice for carcinogenesis model. Those mice were injected with Tamoxifen 2 mg alternate days for 6 timesto activate Cre recombinase in the chief cells.

Results

By activating Cre recombinase, we showed that relatively small number of chief cells was retro-differentiated into neck, parietal, pit and enteroendocrinecells suggesting that chief cells underwent differentiation in exact reverse order to make a complete gland unit. When K-rasG12Dwas activated by pepsinogen C-CreERT2, induction of metaplasia was observed. Addition of p53 knockout with K-rasG12Dinto chief cells showed increasing number of glands with metaplasia. Furthermore, addition of APC knockout combination with K-rasG12Dand p53f/fshowed invasive intestinal type gastric cancer in the corpus. These results suggest that at least small subfraction of chief cell have stem cell activity and potential to give rise to gastric cancer. Recently, new entity of gastric adenocarcinoma has been proposed which called Gastric adenocarcinoma of fundic gland type (chief cell predominant type). We might have showed those type of gastric carcinogenesis.

Conclusions

Chief cell in stomach have stem cell activity and potential to develop gastric cancer.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

The authors.

Funding

Singapore Gastric Cancer Consortium.

Disclosure

All authors have declared no conflicts of interest.

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