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Circulation Research. 2008;103:388-395
Published online before print July 17, 2008, doi: 10.1161/CIRCRESAHA.108.180661
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(Circulation Research. 2008;103:388.)
© 2008 American Heart Association, Inc.

Molecular Medicine

Transcriptional Regulation During Development of the Ductus Arteriosus

Kathryn N. Ivey, David Sutcliffe, James Richardson, Ronald I. Clyman, Joseph A. Garcia, Deepak Srivastava

From the Departments of Pediatrics and Molecular Biology (K.N.I., D. Srivastava), Pathology and Molecular Biology (D. Sutcliffe, J.R.), and Internal Medicine (J.A.G.), University of Texas Southwestern Medical Center, Dallas; and Cardiovascular Research Institute (R.I.C.), Department of Pediatrics, University of California, San Francisco. Present address for K.I. and D. Srivastava: Gladstone Institute of Cardiovascular Disease, University of California, San Francisco.

Correspondence to Deepak Srivastava, Gladstone Institute of Cardiovascular Disease, 1650 Owens St, San Francisco, CA 94158. E-mail dsrivastava{at}gladstone.ucsf.edu

The ductus arteriosus is a specialized blood vessel containing highly differentiated and contractile vascular smooth muscle, derived largely from neural crest cells, that is essential for fetal life but typically closes after birth. Impaired development of the ductus arteriosus or disruption of signaling pathways that initiate postnatal closure can result in persistent patency of the ductus arteriosus, the third most common congenital heart defect. We found that Tfap2β, a transcription factor associated with patent ductus arteriosus in humans, was uniquely expressed in mouse ductal smooth muscle. Endothelin-1 and the hypoxia-induced transcription factor, Hif2{alpha} were also highly enriched in ductal smooth muscle at embryonic day 13.5 and were dependent on Tfap2β for their expression in this domain. Hif2{alpha} functioned as a negative regulator of Tfap2β-induced transcription by disrupting protein–DNA interactions, suggesting a negative feedback loop regulating Tfap2β activity. Our data indicate that Tfap2β, Et-1, and Hif2{alpha} act in a transcriptional network during ductal smooth muscle development and that disruption of this pathway may contribute to patent ductus arteriosus by affecting the development of smooth muscle within the ductus arteriosus.


Key Words: ductus arteriosus • transcriptional regulation • endothelin-1 • Tfap2β • hypoxia-inducible factor 1






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