Modification of Diet to Reduce the Stemness and Tumorigenicity of Murine and Human Intestinal Cells

改变饮食以降低小鼠和人类肠道细胞的干细胞特性和致瘤性

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作者:Stephanie May, Kirsty R Greenow, Adam T Higgins, Anna V Derrick, Elaine Taylor, Pan Pan, Maria Konstantinou, Colin Nixon, Thomas E Wooley, Owen J Sansom, Li-Shu Wang, Lee Parry

Conclusion

BRBs play a role in CRC chemoprevention by protectively regulating the ISC compartment and further supports the use of BRBs in CRC prevention.

Results

Mice with an inducible Apcfl mutation in either the ISC (Lgr5CreERT2 ) or intestinal crypt (AhCre/VillinCreERT2 ) are fed a control or 10% BRB-supplemented diet. This study uses immunohistochemistry, gene expression analysis, and organoid culture to evaluate the effect of BRBs on intestinal homeostasis. RNAscope is performed for ISC markers on CRC adjacent normal colonic tissue pre and post BRB intervention from patients. 10% BRB diet has no overt effect on murine intestinal homeostasis, despite a reduced stem cell number. Following Apc ISC deletion, BRB diet extends lifespan and reduces tumor area. In the AhCre model, BRB diet attenuates the "crypt-progenitor" phenotype and reduces ISC marker gene expression. In ex vivo culture BRBs reduce the self-renewal capacity of murine and human Apc deficient organoids. Finally, the study observes a reduction in ISC marker gene expression in adjacent normal crypts following introduction of BRBs to the human bowel.

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