Sonic hedgehog Signaling from the Urethral Epithelium Controls External Genital Development

Perriton, Claire L.; Powles, Nicola; Chiang, Chin; Maconochie, Mark; Cohn, Martin J.

doi:10.1006/dbio.2002.0668

Cited by 247 publications

(411 citation statements)

References 82 publications

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“…Our results also show that proliferation and Ig secretion by GC B cells are reduced when Hh signaling is inhibited, but these effects are probably the consequence of the decreased GC B cell survival observed. Antiapoptotic effects of Shh have been also demonstrated during development of the nervous system (45), teeth (59), and external genitalia (46), as well as in somite cells (48), keratinocytes (49), thymocytes (60), T lymphocytes (29), and certain neuron populations (47). In GCs, three types of stimuli seem to prevent apoptosis in GC B cells: ligation of the BCR, ligation of CD40, and unknown signals delivered by FDCs (33).…”

Section: Discussionmentioning

confidence: 99%

“…Given that Shh has been described as an antiapoptotic factor for several cell types (29,(45)(46)(47)(48)(49), we decided to examine whether Shh also affected the survival of GC B cells. Isolated GC cells were cultured in the presence or the absence of Hh signaling inhibitors, and the proportion of annexin V-positive dying cells was assessed in the B220 ϩ PNA high GC B cell population.…”

Section: Hh Signaling Blockade Affects Gc B Cell Viabilitymentioning

confidence: 99%

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Sonic Hedgehog Is Produced by Follicular Dendritic Cells and Protects Germinal Center B Cells from Apoptosis

Sacedón¹,

Diez

Nuñez

et al. 2005

The Journal of Immunology

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The Hedgehog (Hh) signaling pathway is involved in the development of many tissues during embryogenesis, but has also been described to function in adult self-renewing tissues. In the immune system, Sonic Hedgehog (Shh) regulates intrathymic T cell development and modulates the effector functions of peripheral CD4+ T cells. In this study we investigate whether Shh signaling is involved in peripheral B cell differentiation in mice. Shh is produced by follicular dendritic cells, mainly in germinal centers (GCs), and GC B cells express both components of the Hh receptor, Patched and Smoothened. Blockade of the Hh signaling pathway reduces the survival, and consequently the proliferation and Ab secretion, of GC B cells. Furthermore, Shh rescues GC B cells from apoptosis induced by Fas ligation. Taken together, our data suggest that Shh is one of the survival signals provided by follicular dendritic cells to prevent apoptosis in GC B cells.

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Section: Discussionmentioning

confidence: 99%

Section: Hh Signaling Blockade Affects Gc B Cell Viabilitymentioning

confidence: 99%

Sonic Hedgehog Is Produced by Follicular Dendritic Cells and Protects Germinal Center B Cells from Apoptosis

Sacedón¹,

Diez

Nuñez

et al. 2005

The Journal of Immunology

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“…The phenotypes of gene knockout mice have revealed that several growth and signaling factor families play fundamental roles in reproductive and urogenital organ formation (Batourina et al, 2002;Doles et al, 2006;Haraguchi et al, 2001;Haraguchi et al, 2000;Huang et al, 2005;Jamin et al, 2002;Kobayashi and Behringer, 2003;Kondo et al, 1996;McMahon et al, 2003;Morgan et al, 2003;Perriton et al, 2002;Suzuki et al, 2003). Shh is expressed in the cloacal epithelia and is vital for the regulation of structures derived from the genital tubercle (GT) and the urogenital sinus, such as the external genitalia and the prostate, respectively (de Santa Barbara and Roberts, 2002;Freestone et al, 2003;Pu et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

“…Shh is expressed in the cloacal epithelia and is vital for the regulation of structures derived from the genital tubercle (GT) and the urogenital sinus, such as the external genitalia and the prostate, respectively (de Santa Barbara and Roberts, 2002;Freestone et al, 2003;Pu et al, 2004). Shh null mouse embryos display GT agenesis associated with aberrant cloacal formation, suggesting that Shh signals emanating from the epithelium of the cloaca may play an essential role in peri-cloacal mesenchyme (PCM) development (Haraguchi et al, 2001;Perriton et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

Molecular analysis of coordinated bladder and urogenital organ formation by Hedgehog signaling

Haraguchi

Motoyama

Sasaki³

et al. 2007

Development

137

162

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The urogenital and reproductive organs, including the external genitalia, bladder and urethra, develop as anatomically aligned organs. Descriptive and experimental embryology suggest that the cloaca, and its derivative, the urogenital sinus, contribute to the formation of these organs. However, it is unknown how the primary tissue lineages in, and adjacent to, the cloaca give rise to the above organs, nor is bladder formation understood. While it is known that sonic hedgehog (Shh) is expressed by the cloacal epithelia, the developmental programs that regulate and coordinate the formation of the urogenital and reproductive organs have not been elucidated. Here we report that Shh mutant embryos display hypoplasia of external genitalia, internal urethra (pelvic urethra) and bladder. The importance of Shh signaling in the development of bladder and external genitalia was confirmed by analyzing a variety of mutant mouse lines with defective hedgehog signaling. By genetically labeling hedgehog-responding tissue lineages adjacent to the cloaca and urogenital sinus, we defined the contribution of these tissues to the bladder and external genitalia. We discovered that development of smooth muscle myosin-positive embryonic bladder mesenchyme requires Shh signaling, and that the bladder mesenchyme and dorsal (upper) external genitalia derive from Shh-responsive peri-cloacal mesenchyme. Thus, the mesenchymal precursors for multiple urogenital structures derive from peri-cloacal mesenchyme and the coordination of urogenital organ formation from these precursors is orchestrated by Shh signals.

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“…Embryonic endoderm gives rise to the bladder urothelium while the connective tissues and smooth muscle of the developing bladder are derived from the peri-cloacal mesenchyme (Haraguchi et al, 2007;Brenner-Anantharam et al, 2007). Genetic studies indicate the homeobox genes play an important role in determining the global patterning of the urogenital system (Satokata et al, 1995;Sciavolino et al, 1997;Warot et al, 1997;Goodman and Scambler, 2001;de Santa and Roberts, 2002;Troy et al, 2003), while key signaling molecules like sonic hedgehog and wnts have been implicated in determining the regional patterning within specific urogenital organs (Perriton et al, 2002;Freestone et al, 2003;Mericskay et al, 2004). The differentiation program responsible for the development of smooth muscle involves the complex interaction of epigenetic and genetic events including chromatin remodeling and acetylation, the SRF-myocar-din pathway, basic helix-loop-helix factors, AP-1 complex genes, and the ternary complex factors of the ETS domain family (Manabe and Owens, 2001;Chen et al, 2002;Du et al, 2003;Kumar and Owens, 2003;Miano, 2003;Wang et al, 2003Wang et al, , 2004Yoshida et al, 2003;Buchwalter et al, 2004;Spin et al, 2004;McDonald et al, 2006;Pipes et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

Transcriptional profiling of the megabladder mouse: A unique model of bladder dysmorphogenesis

Singh¹,

Robinson²,

Ismail³

et al. 2007

Developmental Dynamics

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Recent studies in our lab identified a mutant mouse model of obstructive nephropathy designated mgb for megabladder. Homozygotic mgb mice (mgb؊/؊) develop lower urinary tract obstruction in utero due to a lack of bladder smooth muscle differentiation. This defect is the result of a random transgene insertion/translocation into chromosomes 11 and 16. Transcriptional profiling identified a significantly over-expressed cluster of gene products located on the translocated fragment of chromosome 16 including urotensin II-related peptide (Urp), which was shown to be preferentially over-expressed in developing mgb؊/؊ bladders. Pathway analysis of mgb microarray data indicated dysregulation of at least 60 gene products associated with smooth muscle development. In conclusion, the results of this study indicate that the molecular pathways controlling normal smooth muscle development are severely altered in mgb؊/؊ bladders, and provide the first evidence that Urp may play a critical role in bladder smooth muscle development. Developmental Dynamics 237:170 -186, 2008.

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Sonic hedgehog Signaling from the Urethral Epithelium Controls External Genital Development

Cited by 247 publications

References 82 publications

Sonic Hedgehog Is Produced by Follicular Dendritic Cells and Protects Germinal Center B Cells from Apoptosis

Sonic Hedgehog Is Produced by Follicular Dendritic Cells and Protects Germinal Center B Cells from Apoptosis

Molecular analysis of coordinated bladder and urogenital organ formation by Hedgehog signaling

Transcriptional profiling of the megabladder mouse: A unique model of bladder dysmorphogenesis

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