Requirement of Runx3 in pulmonary vasculogenesis

被引:0
|
作者
Jong-Min Lee
Hyuk-Jae Kwon
Wing-Fu Lai
Han-Sung Jung
机构
[1] Yonsei University,Division in Anatomy and Developmental Biology, Department of Oral Biology, BK21 PLUS project, Oral Science Research Institute, College of Dentistry, Yonsei Center of Biotechnology
[2] The University of Hong Kong,Oral Biosciences, Faculty of Dentistry
[3] Yonsei University,Department of Oral Biology, College of Dentistry
来源
Cell and Tissue Research | 2014年 / 356卷
关键词
Runx3; Lung development; Vasculogenesis; Angiogenesis; Erk signaling;
D O I
暂无
中图分类号
学科分类号
摘要
Runx3 is essential for normal vertebrate lung development and Runx3 knockout (KO) mice die within 24 h after birth because of various organ defects including defects in alveolar expansion. For proper early lung development, vasculogenesis and angiogenesis are necessary in humans. Previous studies have reported that various signaling molecules, such as CD31, VEGF and vWF, are closely related to lung vasculogenesis and angiogenesis. To confirm the relationship between Runx3-related lung defects and vasculogenesis, the localization of various blood vessel markers is examined in WT and Runx3 KO mouse lungs at PN1. Our results indicate that CD31, VEGF and vWF were dramatically up-regulated by a loss of Runx3 during lung development. Moreover, U0126, a MEK inhibitor, rescued the lung phenotype and vascularization by regulation of ERK signaling. Therefore, it was concluded that lung vasculogenesis and angiogenesis were induced in the Runx3 KO mouse, which shows lung defects, by increased CD31, VEGF and vWF.
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页码:445 / 449
页数:4
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