Modulation of morphogenesis by noncanonical Wnt signaling requires ATF/CREB family–mediated transcriptional activation of TGFβ2

被引:0
|
作者
Wenlai Zhou
Lizhu Lin
Arindam Majumdar
Xue Li
Xiaoxue Zhang
Wei Liu
Leah Etheridge
Yunqing Shi
James Martin
Wim Van de Ven
Vesa Kaartinen
Anthony Wynshaw-Boris
Andrew P McMahon
Michael G Rosenfeld
Sylvia M Evans
机构
[1] University of California,Howard Hughes Medical Institute and Department of Medicine
[2] San Diego,Departments of Pharmacology and Medicine
[3] Skaggs School of Pharmacy,Division of Matrix Biology, Department of Medical Biochemistry and Biophysics
[4] University of California,Department of Pediatrics
[5] San Diego,Department of Human Genetics
[6] Karolinska Institute,Department of Pathology
[7] Scheeles väg2,Department of Molecular and Cellular Biology
[8] Plan 4 B1,undefined
[9] Alkek Institute of Biosciences and Technology,undefined
[10] Texas A&M System Health Science Center,undefined
[11] the Comprehensive Cancer Center,undefined
[12] University of California,undefined
[13] San Diego,undefined
[14] Laboratory for Molecular Oncology,undefined
[15] University of Leuven,undefined
[16] Keck School of Medicine,undefined
[17] University of Southern California,undefined
[18] Harvard University,undefined
来源
Nature Genetics | 2007年 / 39卷
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摘要
Transcriptional readout downstream of canonical Wnt signaling is known to be mediated by β-catenin activation of well-described targets, but potential transcriptional readout in response to noncanonical Wnt signaling remains poorly understood. Here, we define a transcriptional pathway important in noncanonical Wnt signaling. We have found that Wnt11 is a direct target of a canonical β-catenin pathway in developing heart and that Wnt11 mutants show cardiac outflow tract defects. We provide genetic and biochemical evidence thatWnt11 signaling affects extracellular matrix composition, cytoskeletal rearrangements and polarized cell movement required for morphogenesis of the cardiac outflow tract. Notably, transforming growth factor β2 (TGFβ2), a key effector of organ morphogenesis, is regulated by Wnt11-mediated noncanonical signaling in developing heart and somites via one or more activating transcription factor (ATF)/cyclic AMP response element binding protein (CREB) family members. Thus, we propose that transcriptional readout mediated at least in part by a Wnt11 → ATF/CREB → TGFβ2 pathway is critical in regulating morphogenesis in response to noncanonical Wnt signaling.
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页码:1225 / 1234
页数:9
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