Identification of a cKit(+) colonic crypt base secretory cell that supports Lgr5(+) stem cells in mice

Michael E Rothenberg; Ysbrand Nusse; Tomer Kalisky; John J Lee; Piero Dalerba; Ferenc Scheeren; Neethan Lobo; Subhash Kulkarni; Sopheak Sim; Dalong Qian; Philip A Beachy; Pankaj J Pasricha; Stephen R Quake; Michael F Clarke

doi:10.1053/j.gastro.2012.02.006

Identification of a cKit(+) colonic crypt base secretory cell that supports Lgr5(+) stem cells in mice

Gastroenterology. 2012 May;142(5):1195-1205.e6. doi: 10.1053/j.gastro.2012.02.006. Epub 2012 Feb 11.

Authors

Michael E Rothenberg¹, Ysbrand Nusse, Tomer Kalisky, John J Lee, Piero Dalerba, Ferenc Scheeren, Neethan Lobo, Subhash Kulkarni, Sopheak Sim, Dalong Qian, Philip A Beachy, Pankaj J Pasricha, Stephen R Quake, Michael F Clarke

Affiliation

¹ Stanford Institute for Stem Cell Biology and Regenerative Medicine, Stanford, California 94305, USA.

Abstract

Background & aims: Paneth cells contribute to the small intestinal niche of Lgr5(+) stem cells. Although the colon also contains Lgr5(+) stem cells, it does not contain Paneth cells. We investigated the existence of colonic Paneth-like cells that have a distinct transcriptional signature and support Lgr5(+) stem cells.

Methods: We used multicolor fluorescence-activated cell sorting to isolate different subregions of colon crypts, based on known markers, from dissociated colonic epithelium of mice. We performed multiplexed single-cell gene expression analysis with quantitative reverse transcriptase polymerase chain reaction followed by hierarchical clustering analysis to characterize distinct cell types. We used immunostaining and fluorescence-activated cell sorting analyses with in vivo administration of a Notch inhibitor and in vitro organoid cultures to characterize different cell types.

Results: Multicolor fluorescence-activated cell sorting could isolate distinct regions of colonic crypts. Four major epithelial subtypes or transcriptional states were revealed by gene expression analysis of selected populations of single cells. One of these, the goblet cells, contained a distinct cKit/CD117(+) crypt base subpopulation that expressed Dll1, Dll4, and epidermal growth factor, similar to Paneth cells, which were also marked by cKit. In the colon, cKit(+) goblet cells were interdigitated with Lgr5(+) stem cells. In vivo, this colonic cKit(+) population was regulated by Notch signaling; administration of a γ-secretase inhibitor to mice increased the number of cKit(+) cells. When isolated from mouse colon, cKit(+) cells promoted formation of organoids from Lgr5(+) stem cells, which expressed Kitl/stem cell factor, the ligand for cKit. When organoids were depleted of cKit(+) cells using a toxin-conjugated antibody, organoid formation decreased.

Conclusions: cKit marks small intestinal Paneth cells and a subset of colonic goblet cells that are regulated by Notch signaling and support Lgr5(+) stem cells.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antigens, CD / analysis
Cell Adhesion Molecules / analysis
Cells, Cultured
Colon / cytology*
Flow Cytometry
Gene Expression Profiling
Goblet Cells / physiology
Hyaluronan Receptors / analysis
Mice
Mice, Inbred C57BL
Paneth Cells / chemistry*
Paneth Cells / physiology*
Proto-Oncogene Proteins c-kit / analysis*
Receptors, G-Protein-Coupled / analysis*
Receptors, Notch / physiology
Single-Cell Analysis
Stem Cells / chemistry
Stem Cells / physiology*

Substances

Antigens, CD
CD66 antigens
Cell Adhesion Molecules
Hyaluronan Receptors
Lgr5 protein, mouse
Receptors, G-Protein-Coupled
Receptors, Notch
Proto-Oncogene Proteins c-kit

Abstract

Publication types

MeSH terms

Substances

Grants and funding