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Involvement of the Reck tumor suppressor protein in maternal and embryonic vascular remodeling in mice

Authors
Chandana, Ediriweera P. S.Maeda, YasuhiroUeda, AkihikoKiyonari, HiroshiOshima, NaokoYamamoto, MakoKondo, ShunyaOh, JunseoTakahashi, ReiYoshida, YokoKawashima, SatoshiAlexander, David B.Kitayama, HitoshiTakahashi, ChiakiTabata, YasuhikoMatsuzaki, TomokoNoda, Makoto
Issue Date
6-Aug-2010
Publisher
BMC
Citation
BMC DEVELOPMENTAL BIOLOGY, v.10
Indexed
SCIE
SCOPUS
Journal Title
BMC DEVELOPMENTAL BIOLOGY
Volume
10
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/115894
DOI
10.1186/1471-213X-10-84
ISSN
1471-213X
Abstract
Background: Developmental angiogenesis proceeds through multiple morphogenetic events including sprouting, intussusception, and pruning. Mice lacking the membrane-anchored metalloproteinase regulator Reck die in utero around embryonic day 10.5 with halted vascular development; however, the mechanisms by which this phenotype arises remain unclear. Results: We found that Reck is abundantly expressed in the cells associated with blood vessels undergoing angiogenesis or remodelling in the uteri of pregnant female mice. Some of the Reck-positive vessels show morphological features consistent with non-sprouting angiogenesis. Treatment with a vector expressing a small hairpin RNA against Reck severely disrupts the formation of blood vessels with a compact, round lumen. Similar defects were found in the vasculature of Reck-deficient or Reck conditional knockout embryos. Conclusions: Our findings implicate Reck in vascular remodeling, possibly through non-sprouting angiogenesis, in both maternal and embyornic tissues.
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