2016
DOI: 10.1093/ecco-jcc/jjw212
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Inducible Colonic M Cells Are Dependent on TNFR2 but Not Ltβr, Identifying Distinct Signalling Requirements for Constitutive Versus Inducible M Cells

Abstract: TNFR2 is required for inflammation-inducible M cells, indicating that constitutive versus inflammation-inducible M cells depend on different triggers. The inducible M cell dependence on TNFR2 suggests that this specific subset is dependent on TNFα in addition to a presumed requirement for RANKL. Since inducible M cell function will influence immune responses, selective blockade of TNFα may affect colonic inflammation.

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Cited by 9 publications
(13 citation statements)
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“…At present, the mechanisms by which inflammatory cytokines and infectious models (such as Salmonella and C. rodentium ) induce M-cells are not well-understood 5153 . Overexpression of p52-RelB failed to induce M-cells and similarly, constitutive epithelial NIK signaling was not sufficient to increase M-cells in PP or colon LF.…”
Section: Discussionmentioning
confidence: 99%
“…At present, the mechanisms by which inflammatory cytokines and infectious models (such as Salmonella and C. rodentium ) induce M-cells are not well-understood 5153 . Overexpression of p52-RelB failed to induce M-cells and similarly, constitutive epithelial NIK signaling was not sufficient to increase M-cells in PP or colon LF.…”
Section: Discussionmentioning
confidence: 99%
“…Yet another subset of stromal cells in a discrete layer below the FAE expresses the cytokine RANKL (92, 93). This cytokine has been shown to correlate with M cell induction, and in organoid cultures, addition of exogenous RANKL was sufficient to induce functional M cell development (31, 33, 9496).…”
Section: Organized Lymphoid Tissues and The Life History Of “Constitumentioning
confidence: 98%
“…Moreover, while organoid cultures confirm the requirement for RANKL in M cell induction, the location of RANKL+ stromal cells in Peyer's patches is curious. Instead of being located immediately adjacent to the crypts, they appear to be predominantly in the subepithelial dome region (96) (Figure 5). Thus, while RANKL may have a role in crypt cell induction and lineage commitment (Step 1 in the two step model), the anatomy of RANKL expression suggests that RANKL, instead of being simply an early inducer of crypt stem cells, may also provide reinforcement of an early M cell lineage commitment (induced how?…”
Section: Organized Lymphoid Tissues and The Life History Of “Constitumentioning
confidence: 99%
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