4.4 Article

Co-Culture of Murine Small Intestine Epithelial Organoids with Innate Lymphoid Cells

Journal

JOVE-JOURNAL OF VISUALIZED EXPERIMENTS
Volume -, Issue 181, Pages -

Publisher

JOURNAL OF VISUALIZED EXPERIMENTS
DOI: 10.3791/63554

Keywords

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Funding

  1. Wellcome Trust [215027/Z/18/Z, 203757/Z/16/A, 204394/Z/16/Z]
  2. NIHR GSTT BRC
  3. Marie Sklodowska-Curie Fellowship
  4. RCUK/UKRI Rutherford Fund fellowship [MR/R024812/1]
  5. King's Prize fellowship
  6. Wellcome Trust [204394/Z/16/Z, 203757/Z/16/A] Funding Source: Wellcome Trust

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Co-cultures of organoids with immune cells offer a versatile tool for studying mucosal homeostasis, providing insights into the interactions between epithelial and immune cells.
Complex co-cultures of organoids with immune cells provide a versatile tool for interrogating the bi-directional interactions that underpin the delicate balance of mucosal homeostasis. These 3D, multi-cellular systems offer a reductionist model for addressing multi-factorial diseases and resolving technical difficulties that arise when studying rare cell types such as tissue-resident innate lymphoid cells (ILCs). This article describes a murine system that combines small intestine organoids and small intestine lamina propria derived helper-like type-1 ILCs (ILC1s), which can be readily extended to other ILC or immune populations. ILCs are a tissue-resident population that is particularly enriched in the mucosa, where they promote homeostasis and rapidly respond to damage or infection. Organoid co-cultures with ILCs have already begun shedding light on new epithelial-immune signaling modules in the gut, revealing how different ILC subsets impact intestinal epithelial barrier integrity and regeneration. This protocol will enable further investigations into reciprocal interactions between epithelial and immune cells, which hold the potential to provide new insights into the mechanisms of mucosal homeostasis and inflammation.

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