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Publication : Mice deficient for BMP2 are nonviable and have defects in amnion/chorion and cardiac development.

First Author  Zhang H Year  1996
Journal  Development Volume  122
Issue  10 Pages  2977-86
PubMed ID  8898212 Mgi Jnum  J:36213
Mgi Id  MGI:83651 Doi  10.1242/dev.122.10.2977
Citation  Zhang H, et al. (1996) Mice deficient for BMP2 are nonviable and have defects in amnion/chorion and cardiac development. Development 122(10):2977-86
abstractText  To address the function of bone morphogenetic protein-2 (BMP2) in mammalian development, mice with a targeted deletion of the Bmp2 mature region were generated using embryonic stem cell technology. This mutation caused embryonic lethality when homozygous. Mutant embryos failed to close the proamniotic canal, which caused the malformation of the amnion/chorion. BMP2-deficient embryos also exhibited a defect in cardiac development, manifested by the abnormal development of the heart in the exocoelomic cavity. These defects are consistent with the expression of Bmp2 in the extraembryonic mesoderm cells and promyocardium. Thus BMP2 is a critical factor for both extraembryonic and embryonic development.
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