- 作者:Yu-Hwai Tsai1 ; David R. Hill1 ; Namit Kumar2 ; Sha Huang1 ; Alana M. Chin3 ; Briana R. Dye3 ; Melinda S. Nagy1 ; Michael P. Verzi2 ; Jason R. Spence1 ; 3 ; 4 ; spencejr@umich.edu" class="auth_mail" title="E-mail the corresponding author
- 关键词:Pluripotent Stem Cells ; Endoderm ; LGR5 ; WNT ; Organoid ; Intestine
- 刊名:CMGH Cellular and Molecular Gastroenterology and Hepatology
- 出版年:2016
- 出版时间:September 2016
- 年:2016
- 卷:2
- 期:5
- 页码:648-662.e8
- 全文大小:13271 K
Methods
ra0015">We interrogated the function and expression of LGR family members using human pluripotent stem cell–derived tissues including definitive endoderm, mid/hindgut, and intestinal organoids. We performed embryonic lineage tracing in Lgr5-GFP-IRES-CreERT2 mice.
Results
ra0020">We show that LGR5 is part of the human definitive endoderm (DE) gene signature, and LGR5 transcripts are induced robustly when human pluripotent stem cells are differentiated into DE. Our results show that LGR4 and 5 are functionally required for efficient human endoderm induction. Consistent with data in human DE, we observe Lgr5 reporter (eGFP) activity in the embryonic day 8.5 mouse endoderm, and show the ability to lineage trace these cells into the adult intestine. However, gene expression data also suggest that there are human–mouse species-specific differences at later time points of embryonic development.
Conclusions
ra0025">Our results show that LGR5 is induced during DE differentiation, LGR receptors are functionally required for DE induction, and that they function to potentiate WNT signaling during this process.