Organoids capture tissue-specific innate lymphoid cell development in mice and humans

类器官捕获小鼠和人类组织特异性先天淋巴细胞的发育

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作者:Geraldine M Jowett, Emily Read, Luke B Roberts, Diana Coman, Marta Vilà González, Tomasz Zabinski, Umar Niazi, Rita Reis, Tung-Jui Trieu, Davide Danovi, Eileen Gentleman, Ludovic Vallier, Michael A Curtis, Graham M Lord, Joana F Neves

Abstract

Organoid-based models of murine and human innate lymphoid cell precursor (ILCP) maturation are presented. First, murine intestinal and pulmonary organoids are harnessed to demonstrate that the epithelial niche is sufficient to drive tissue-specific maturation of all innate lymphoid cell (ILC) groups in parallel, without requiring subset-specific cytokine supplementation. Then, more complex human induced pluripotent stem cell (hiPSC)-based gut and lung organoid models are used to demonstrate that human epithelial cells recapitulate maturation of ILC from a stringent systemic human ILCP population, but only when the organoid-associated stromal cells are depleted. These systems offer versatile and reductionist models to dissect the impact of environmental and mucosal niche cues on ILC maturation. In the future, these could provide insight into how ILC activity and development might become dysregulated in chronic inflammatory diseases.

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