Literature DB >> 23429912

TCDD inhibition of canonical Wnt signaling disrupts prostatic bud formation in mouse urogenital sinus.

Amanda M Branam1, Nicole M Davis, Robert W Moore, Andrew J Schneider, Chad M Vezina, Richard E Peterson.   

Abstract

In mice, in utero exposure to 2,3,7,8-tetrachlorodibenzo-p- dioxin (TCDD) reduces the number of dorsolateral prostatic buds resulting in a smaller dorsolateral prostate and prevents formation of ventral buds culminating in ventral prostate agenesis. The genes and signaling pathways affected by TCDD that are responsible for disrupting prostate development are largely unknown. Here we show that treatment of urogenital sinus (UGS) organ cultures with known inhibitors of canonical Wnt signaling also inhibits prostatic bud formation. In support of the hypothesis that TCDD decreases canonical Wnt signaling, we identify inhibitory effects of TCDD on multiple components of the canonical Wnt signaling pathway in the UGS that temporally coincide with the inhibitory effect of TCDD on prostatic bud formation: (1) expression of R-spondins (Rspo2 and Rspo3) that promote canonical Wnt signaling is reduced; (2) expression of Lef1, Tcf1, and Wif1, established canonical Wnt target genes, is decreased; (3) expression of Lgr5, a RSPO receptor that activates canonical Wnt signaling, is reduced; and (4) expression of Dickkopfs (Dkks), inhibitors of canonical Wnt signaling, is not increased by TCDD. Thus, the TCDD-induced reduction in canonical Wnt signaling is associated with a decrease in activators (Rspo2 and Rspo3) rather than an increase in inhibitors (Dkk1 and Dkk2) of the pathway. This study focuses on determining whether treatment of TCDD-exposed UGS organ cultures with RSPO2 and/or RSPO3 is capable of rescuing the inhibitory effects of TCDD on canonical Wnt signaling and prostatic bud formation. We discovered that each RSPO alone or in combination partially rescues TCDD inhibition of both canonical Wnt signaling and prostatic bud formation.

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Year:  2013        PMID: 23429912      PMCID: PMC3627553          DOI: 10.1093/toxsci/kft027

Source DB:  PubMed          Journal:  Toxicol Sci        ISSN: 1096-0929            Impact factor:   4.849


  44 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2001-12-18       Impact factor: 11.205

2.  Stromal-epithelial interactions--I. Induction of prostatic phenotype in urothelium of testicular feminized (Tfm/y) mice.

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4.  Evidence that inhibited prostatic epithelial bud formation in 2,3,7,8-tetrachlorodibenzo-p-dioxin-exposed C57BL/6J fetal mice is not due to interruption of androgen signaling in the urogenital sinus.

Authors:  Kinarm Ko; H Michael Theobald; Robert W Moore; Richard E Peterson
Journal:  Toxicol Sci       Date:  2004-03-31       Impact factor: 4.849

5.  Aryl hydrocarbon receptors in urogenital sinus mesenchyme mediate the inhibition of prostatic epithelial bud formation by 2,3,7,8-tetrachlorodibenzo-p-dioxin.

Authors:  Kinarm Ko; Robert W Moore; Richard E Peterson
Journal:  Toxicol Appl Pharmacol       Date:  2004-04-01       Impact factor: 4.219

6.  In utero and lactational exposure to 2,3,7,8-tetrachlorodibenzo-p-dioxin in the C57BL/6J mouse prostate: lobe-specific effects on branching morphogenesis.

Authors:  Kinarm Ko; H Michael Theobald; Richard E Peterson
Journal:  Toxicol Sci       Date:  2002-12       Impact factor: 4.849

7.  Region-specific inhibition of prostatic epithelial bud formation in the urogenital sinus of C57BL/6 mice exposed in utero to 2,3,7,8-tetrachlorodibenzo-p-dioxin.

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8.  Beta-catenin (CTNNB1) induces Bmp expression in urogenital sinus epithelium and participates in prostatic bud initiation and patterning.

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10.  FGF-10 plays an essential role in the growth of the fetal prostate.

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Journal:  Dev Biol       Date:  2003-09-01       Impact factor: 3.582

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  11 in total

Review 1.  Prostate organogenesis: tissue induction, hormonal regulation and cell type specification.

Authors:  Roxanne Toivanen; Michael M Shen
Journal:  Development       Date:  2017-04-15       Impact factor: 6.868

2.  In utero exposure to TCDD alters Wnt signaling during mouse prostate development: linking ventral prostate agenesis to downregulated β-catenin signaling.

Authors:  Andrew J Schneider; Robert W Moore; Amanda M Branam; Lisa L Abler; Kimberly P Keil; Vatsal Mehta; Chad M Vezina; Richard E Peterson
Journal:  Toxicol Sci       Date:  2014-06-13       Impact factor: 4.849

3.  Combination effects of AHR agonists and Wnt/β-catenin modulators in zebrafish embryos: Implications for physiological and toxicological AHR functions.

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Review 4.  Recent advances in understanding the pathogenesis of scleroderma-interstitial lung disease.

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5.  Prostate cancer reactivates developmental epigenomic programs during metastatic progression.

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Journal:  Nat Genet       Date:  2020-07-20       Impact factor: 38.330

6.  Biological significance and therapeutic implication of resveratrol-inhibited Wnt, Notch and STAT3 signaling in cervical cancer cells.

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Journal:  Genes Cancer       Date:  2014-05

Review 7.  Environmental Ligands of the Aryl Hydrocarbon Receptor and Their Effects in Models of Adult Liver Progenitor Cells.

Authors:  Jan Vondráček; Miroslav Machala
Journal:  Stem Cells Int       Date:  2016-05-04       Impact factor: 5.443

8.  Signaling Events Downstream of AHR Activation That Contribute to Toxic Responses: The Functional Role of an AHR-Dependent Long Noncoding RNA (slincR) Using the Zebrafish Model.

Authors:  Gloria R Garcia; Prarthana Shankar; Cheryl L Dunham; Abraham Garcia; Jane K La Du; Lisa Truong; Susan C Tilton; Robert L Tanguay
Journal:  Environ Health Perspect       Date:  2018-11       Impact factor: 9.031

Review 9.  Intersection of AHR and Wnt signaling in development, health, and disease.

Authors:  Andrew J Schneider; Amanda M Branam; Richard E Peterson
Journal:  Int J Mol Sci       Date:  2014-10-03       Impact factor: 5.923

10.  Insight into the relationship between aryl-hydrocarbon receptor and β-catenin in human colon cancer cells.

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Journal:  PLoS One       Date:  2019-11-01       Impact factor: 3.240

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