Peyer's patch M cells derived from Lgr5(+) stem cells require SpiB and are induced by RankL in cultured "miniguts".
Publication date
2012
Authors
Kajuala, P.
Nieuwenhuis, E.E.S.
Schneeberger, K.
Middendorp, S.
Barker, N.
Li, S.
Martens, A.C.M.
Hofhuis, F.M.A.
DeKoter, R.P.
Peters, P.J.
Editors
Advisors
Supervisors
Document Type
Article
Metadata
Show full item recordCollections
License
(c) UU Universiteit Utrecht, 2012
Abstract
Peyer’s patches consist of domains of specialized intestinal epithelium overlying gut-associated lymphoid tissue (GALT). Luminal
antigens reach the GALT by translocation through epithelial gatekeeper cells, the so-calledMcells. We recently demonstrated
that all epithelial cells required for the digestive functions of the intestine are generated from Lgr5-expressing stem cells.
Here, we show thatMcells also derive from these crypt-based Lgr5 stem cells. The Ets family transcription factor SpiB, known to
control effector functions of bone marrow-derived immune cells, is specifically expressed inMcells. In SpiB / mice,Mcells are
entirely absent, which occurs in a cell-autonomous fashion. It has been shown that Tnfsf11 (RankL) can induceMcell development
in vivo. We show that in intestinal organoid (“minigut”) cultures, stimulation with RankL induces SpiB expression within
24 h and expression of otherMcell markers subsequently. We conclude that RankL-induced expression of SpiB is essential for
Lgr5 stem cell-derived epithelial precursors to develop intoMcells.