Regulation of Prostate Branching Morphogenesis by Activin A and Follistatin

Ventral prostate development occurs by branching morphogenesis and is an androgen-dependent process modulated by growth factors. Many growth factors have been implicated in branching morphogenesis including activins (dimers of βA and βB subunits); activin A inhibited branching of lung and kidney in...

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Bibliographic Details
Published in:Developmental biology 2001-09, Vol.237 (1), p.145-158
Main Authors: Cancilla, Belinda, Jarred, Renea A, Wang, Hong, Mellor, Sally L, Cunha, Gerald R, Risbridger, Gail P
Format: Article
Language:English
Subjects:
activin
Activin Receptors
Activins
Animals
branching morphogenesis
Follistatin
Glycoproteins - analysis
Glycoproteins - pharmacology
Immunohistochemistry
Inhibin-beta Subunits
Inhibins - analysis
Inhibins - genetics
Inhibins - pharmacology
Male
Morphogenesis - drug effects
Organ Culture Techniques
Peptides - analysis
prostate
Prostate - embryology
Rats
Rats, Sprague-Dawley
Receptors, Growth Factor - analysis
RNA, Messenger - analysis
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Summary:Ventral prostate development occurs by branching morphogenesis and is an androgen-dependent process modulated by growth factors. Many growth factors have been implicated in branching morphogenesis including activins (dimers of βA and βB subunits); activin A inhibited branching of lung and kidney in vitro. Our aim was to examine the role of activins on prostatic development in vitro and their localization in vivo. Organ culture of day 0 rat ventral prostates for 6 days with activin A (+/− testosterone) inhibited prostatic branching and growth without increasing apoptosis. The activin-binding protein follistatin increased branching in vitro in the absence (but not presence) of testosterone, suggesting endogenous activins may reduce prostatic branching morphogenesis. In vivo, inhibin α subunit was not expressed until puberty, therefore inhibins (dimers of α and β subunits) are not involved in prostatic development. Activin βA was immunolocalized to developing prostatic epithelium and mesenchymal aggregates at ductal tips. Activin βB immunoreactivity was weak during development, but was upregulated in prostatic epithelium during puberty. Activin receptors were expressed throughout the prostatic epithelium. Follistatin mRNA and protein were expressed throughout the prostatic epithelium. The in vitro evidence that activin and follistatin have opposing effects on ductal branching suggests a role for activin as a negative regulator of prostatic ductal branching morphogenesis.
ISSN:0012-1606
1095-564X
DOI:10.1006/dbio.2001.0364