Wen L , Hasebe T , Miller TC , Ishizuya-Oka A , Shi YB .

	Figure 1. Inhibition of hedgehog (Shh) signaling by cyclopamine suppresses intestinal remodeling during Xenopus laevis metamorphosis . A: Cyclopamine-treated animals have longer intestine at the end of metamorphosis. Tadpoles at stage 58 were treated with vehicle (100% ethanol, final concentration in rearing water: 0.1%) (3 tadpoles) or tomatidine (7 tadpoles), or cyclopamine (8 tadpoles) till they reached stage 66. Intestinal length was measured from bile duct junction to colon for all animals. * indicated significant difference between the cyclopamine group and the other two groups (p < 0.05). Note that the cyclopamine-treated tadpoles completed metamorphosis, as judged based on external morphology, e.g., resorption of the tail, similarly as the animals in the tomatidine and vehicle groups. However, they had significant longer intestine. B: Retarded intestinal maturation in the cyclopamine-treated animals. Transverse sections of the intestine from the animals above were stained with methyl green pyronin Y (MGPY), which stained DNA in blue (methyl green) and RNA in red (pyronin Y). Note that the cyclopamine-treated animals had intestines with fewer and less structured epithelial folds as well as reduced connective tissue and muscles (outer layers). C: Immunofluorescence staining showing reduced intestinal muscle development in the cyclopamine-treated animals. The intestinal sections above were stained with anti-smooth muscle actin (SMA) antibody as well as DAPI for cell nuclei.
	Figure 2. Inhibition of hedgehog signaling suppresses intestine shortening and remodeling at metamorphic climax. A: Cyclopamine-treated tadpoles have longer intestine at the climax. Tadpoles at stage 58 were treated with vehicle (100% ethanol, final concentration in rearing water: 0.1%) (9 tadpoles) or tomatidine (10 tadpoles), or cyclopamine (11 tadpoles) till they reached climax (stage 62). Intestine was isolated and measured from bile duct junction to colon. The animals in all three groups reached developed to stage 62 similarly as judged based on external morphology. ** indicate significant difference between the cyclopamine group and the two control groups (p < 0.001). B: Cyclopamine-treated tadpoles have fewer islets of adult epithelial stem cells. Transverse sections of the intestine from above were stained with methyl green pyronin Y (MGPY). The boxed area in the left panel is enlarged in the right panel. Note that at the climax of metamorphosis, the clusters (islets) of adult epithelial stem cells are stained strongly by MGPY (arrows) while the dying larval epithelial cells are only weakly stained [15,49,50]. The cyclopamine-treated tadpoles had smaller intestinal cross-section and fewer islets of adult cells. C: Cyclopamine-treated tadpoles have reduced cell proliferation. The intestinal sections above were stained with DAPI for nuclear DNA and anti-PCNA antibody for mitotic cells. The boxed area in the middle panel is enlarged in the right panel. Cyclopamine treatment significantly reduced cell proliferation in the intestine, especially in the epithelium. Note that the labeling in the epithelium was limited to the islet of the adult cells (arrows) but not in the dying larval epithelial cells, as expected.
	Figure 3. Cyclopamine inhibits Shh target gene expression. Tadpoles at stage 58 were treated as in Figure 2 until they reached stage 62. Total intestinal RNA was isolated for qRT-PCR analysis of the expression of Shh target genes BMP4 [51] (A), Snai2 [52] (B) and Twist1 [52] (C). ** indicate significant difference between the cyclopamine group and the other groups (p < 0.001).
	Figure 4. Snai2 expression is restricted to the connective tissue and peaks at the climax of intestinal metamorphosis. A: Snai2 mRNA level peaks at the climax (Stage 62). Quantitative RT-PCR analysis of Snai2 mRNA level in intestine from tadpoles at indicated stages, normalized against the control gene EF1a. B-G: In situ hybridization reveals connective tissue-specific expression of Snai2 in intestine. Note that high levels of Snai2 mRNA were detected fairly uniformly in the connective tissue at the climax (St61-62). H-I: Snai2 is not expressed in the muscle layers. In situ hybridization sections of Snai2 at the stage 61 were double-stained with smooth muscle actin antibody (red) to label the muscle layers (Ms). Ty: typhlosole, the single epithelial fold in in premetamorphic tadpole intestine where connective tissue is abundant; Lu: lumen; Ep: epithelium. Note that Snai2 labeled cells are localized between epithelium and muscle layers.
	Figure 5. Twist1 has similar spatiotemporal expression profiles as Snai2 in the intestine. A: Twist1 mRNA level peaks at the climax (Stage 62). Quantitative RT-PCR analysis of Twist1 mRNA level in intestine from tadpoles at indicated stages, normalized against the control gene EF1a. B-G: In situ hybridization reveals connective tissue-specific expression of Twist1 in intestine. Note that Twist1 mRNA level peaked in the connective tissue at the climax (St61-62). H-I: Twist1 is not expressed in the muscle layers. In situ hybridization sections of Twist1 at the stage 61 were double-stained with smooth muscle actin antibody (red) to labeled the muscle layers (Ms). Ty: typhlosole, the single epithelial fold in in premetamorphic tadpole intestine where connective tissue is abundant; Lu: lumen; Ep: epithelium. Note that Twist1 labeled cells are localized between epithelium and muscle layers.
	Figure 6. A schematic diagram showing the effects of Shh signaling during intestinal remodeling. Shh appears to enhance the proliferation of cells in all three tissue layers during metamorphosis. Shh receptors and downstream transcription factors are highly expressed in the connective tissue, which are likely responsible for the activation of the expression of BMP-4, Snai2, and Twist1. The connective tissue may in turn help to mediate the cell proliferation effects of Shh on the adult epithelial stem cells and the circular muscle cells. Cyclopamine directly inhibits Shh signaling in the epithelium and thus blocks all the effects of Shh.

Blitz, Biallelic genome modification in F(0) Xenopus tropicalis embryos using the CRISPR/Cas system. 2013, Pubmed, Xenbase

Blitz, Biallelic genome modification in F(0) Xenopus tropicalis embryos using the CRISPR/Cas system. 2013, Pubmed , Xenbase
Brown, Amphibian metamorphosis. 2007, Pubmed , Xenbase
Buchholz, Pairing morphology with gene expression in thyroid hormone-induced intestinal remodeling and identification of a core set of TH-induced genes across tadpole tissues. 2007, Pubmed , Xenbase
Buchholz, Molecular and developmental analyses of thyroid hormone receptor function in Xenopus laevis, the African clawed frog. 2006, Pubmed , Xenbase
Burke, Co-repressors 2000. 2000, Pubmed
Chen, Inhibition of Hedgehog signaling by direct binding of cyclopamine to Smoothened. 2002, Pubmed
Cooper, Teratogen-mediated inhibition of target tissue response to Shh signaling. 1998, Pubmed
Das, Identification of direct thyroid hormone response genes reveals the earliest gene regulation programs during frog metamorphosis. 2009, Pubmed , Xenbase
Denver, Neuroendocrinology of amphibian metamorphosis. 2013, Pubmed
Fu, A causative role of stromelysin-3 in extracellular matrix remodeling and epithelial apoptosis during intestinal metamorphosis in Xenopus laevis. 2005, Pubmed , Xenbase
Glass, The coregulator exchange in transcriptional functions of nuclear receptors. 2000, Pubmed
Guo, Efficient RNA/Cas9-mediated genome editing in Xenopus tropicalis. 2014, Pubmed , Xenbase
Harper, The transcriptional repressor Blimp1/Prdm1 regulates postnatal reprogramming of intestinal enterocytes. 2011, Pubmed
Hasebe, Epithelial-connective tissue interactions induced by thyroid hormone receptor are essential for adult stem cell development in the Xenopus laevis intestine. 2011, Pubmed , Xenbase
Hasebe, Thyroid hormone-induced cell-cell interactions are required for the development of adult intestinal stem cells. 2013, Pubmed , Xenbase
Hasebe, Thyroid hormone-induced sonic hedgehog signal up-regulates its own pathway in a paracrine manner in the Xenopus laevis intestine during metamorphosis. 2012, Pubmed , Xenbase
Heimeier, Studies on Xenopus laevis intestine reveal biological pathways underlying vertebrate gut adaptation from embryo to adult. 2010, Pubmed , Xenbase
Ishizuya-Oka, Thyroid hormone-upregulated expression of Musashi-1 is specific for progenitor cells of the adult epithelium during amphibian gastrointestinal remodeling. 2003, Pubmed , Xenbase
Ishizuya-Oka, Shh/BMP-4 signaling pathway is essential for intestinal epithelial development during Xenopus larval-to-adult remodeling. 2006, Pubmed , Xenbase
Ishizuya-Oka, Origin of the adult intestinal stem cells induced by thyroid hormone in Xenopus laevis. 2009, Pubmed , Xenbase
Ishizuya-Oka, Thyroid hormone-induced expression of sonic hedgehog correlates with adult epithelial development during remodeling of the Xenopus stomach and intestine. 2001, Pubmed , Xenbase
Ishizuya-Oka, Evolutionary insights into postembryonic development of adult intestinal stem cells. 2011, Pubmed
Ishizuya-Oka, Apoptosis and cell proliferation in the Xenopus small intestine during metamorphosis. 1996, Pubmed , Xenbase
Ishizuya-Oka, Connective tissue is involved in adult epithelial development of the small intestine during anuran metamorphosis in vitro. 1992, Pubmed
Jones, Multiple N-CoR complexes contain distinct histone deacetylases. 2001, Pubmed , Xenbase
Jones, N-CoR-HDAC corepressor complexes: roles in transcriptional regulation by nuclear hormone receptors. 2003, Pubmed , Xenbase
Katoh, Hedgehog target genes: mechanisms of carcinogenesis induced by aberrant hedgehog signaling activation. 2009, Pubmed
Lazar, Thyroid hormone receptors: multiple forms, multiple possibilities. 1993, Pubmed
Lei, Generation of gene disruptions by transcription activator-like effector nucleases (TALENs) in Xenopus tropicalis embryos. 2013, Pubmed , Xenbase
Marigo, Biochemical evidence that patched is the Hedgehog receptor. 1996, Pubmed , Xenbase
Matsuda, An essential and evolutionarily conserved role of protein arginine methyltransferase 1 for adult intestinal stem cells during postembryonic development. 2010, Pubmed , Xenbase
McKenna, Nuclear receptors, coregulators, ligands, and selective receptor modulators: making sense of the patchwork quilt. 2001, Pubmed
Muncan, Blimp1 regulates the transition of neonatal to adult intestinal epithelium. 2011, Pubmed
Nakayama, Simple and efficient CRISPR/Cas9-mediated targeted mutagenesis in Xenopus tropicalis. 2013, Pubmed , Xenbase
Rachez, Mediator complexes and transcription. 2001, Pubmed
Roberts, Sonic hedgehog is an endodermal signal inducing Bmp-4 and Hox genes during induction and regionalization of the chick hindgut. 1995, Pubmed
Ruiz i Altaba, Catching a Gli-mpse of Hedgehog. 1997, Pubmed
Schreiber, Remodeling of the intestine during metamorphosis of Xenopus laevis. 2005, Pubmed , Xenbase
Schreiber, Cell-cell interactions during remodeling of the intestine at metamorphosis in Xenopus laevis. 2009, Pubmed , Xenbase
Shi, Thyroid hormone regulation of apoptotic tissue remodeling: implications from molecular analysis of amphibian metamorphosis. 2001, Pubmed , Xenbase
Shi, The earliest changes in gene expression in tadpole intestine induced by thyroid hormone. 1993, Pubmed , Xenbase
Shi, Tadpole competence and tissue-specific temporal regulation of amphibian metamorphosis: roles of thyroid hormone and its receptors. 1996, Pubmed , Xenbase
Shi, Biphasic intestinal development in amphibians: embryogenesis and remodeling during metamorphosis. 1996, Pubmed , Xenbase
Shi, Unliganded thyroid hormone receptor regulates metamorphic timing via the recruitment of histone deacetylase complexes. 2013, Pubmed , Xenbase
Shi, Thyroid hormone receptor actions on transcription in amphibia: The roles of histone modification and chromatin disruption. 2012, Pubmed
Stolow, Xenopus sonic hedgehog as a potential morphogen during embryogenesis and thyroid hormone-dependent metamorphosis. 1995, Pubmed , Xenbase
Su, Thyroid hormone induces apoptosis in primary cell cultures of tadpole intestine: cell type specificity and effects of extracellular matrix. 1997, Pubmed , Xenbase
Sukegawa, The concentric structure of the developing gut is regulated by Sonic hedgehog derived from endodermal epithelium. 2000, Pubmed
Sun, Thyroid hormone regulation of adult intestinal stem cell development: mechanisms and evolutionary conservations. 2012, Pubmed , Xenbase
Sun, Expression profiling of intestinal tissues implicates tissue-specific genes and pathways essential for thyroid hormone-induced adult stem cell development. 2013, Pubmed , Xenbase
Sun, Epigenetic regulation of thyroid hormone-induced adult intestinal stem cell development during anuran metamorphosis. 2014, Pubmed , Xenbase
Sun, Spatio-temporal expression profile of stem cell-associated gene LGR5 in the intestine during thyroid hormone-dependent metamorphosis in Xenopus laevis. 2010, Pubmed , Xenbase
Tabin, Recent advances in hedgehog signalling. 1997, Pubmed
Tata, Gene expression during metamorphosis: an ideal model for post-embryonic development. 1993, Pubmed
Tsai, Molecular mechanisms of action of steroid/thyroid receptor superfamily members. 1994, Pubmed
Wen, Histone methyltransferase Dot1L plays a role in postembryonic development in Xenopus tropicalis. 2015, Pubmed , Xenbase
Wong, Coordinated regulation of and transcriptional activation by Xenopus thyroid hormone and retinoid X receptors. 1995, Pubmed , Xenbase
Wong, A role for nucleosome assembly in both silencing and activation of the Xenopus TR beta A gene by the thyroid hormone receptor. 1995, Pubmed , Xenbase
Yen, Physiological and molecular basis of thyroid hormone action. 2001, Pubmed
Zhang, The mechanism of action of thyroid hormones. 2000, Pubmed
van den Brink, Hedgehog signaling in development and homeostasis of the gastrointestinal tract. 2007, Pubmed