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Literature DB >> 25271168

Global ablation of the mouse Rab11a gene impairs early embryogenesis and matrix metalloproteinase secretion.

Shiyan Yu¹, Ghassan Yehia², Juanfei Wang³, Ewa Stypulkowski¹, Ryotaro Sakamori¹, Ping Jiang⁴, Berenice Hernandez-Enriquez¹, Tracy S Tran¹, Edward M Bonder¹, Wei Guo³, Nan Gao⁵.

Abstract

Rab11a has been conceived as a prominent regulatory component of the recycling endosome, which acts as a nexus in the endo- and exocytotic networks. The precise in vivo role of Rab11a in mouse embryonic development is unknown. We globally ablated Rab11a and examined the phenotypic and molecular outcomes in Rab11a(null) blastocysts and mouse embryonic fibroblasts. Using multiple trafficking assays and complementation analyses, we determined, among multiple important membrane-associated and soluble cargos, the critical contribution of Rab11a vesicular traffic to the secretion of multiple soluble MMPs. Rab11a(null) embryos were able to properly form normal blastocysts but died at peri-implantation stages. Our data suggest that Rab11a critically controls mouse blastocyst development and soluble matrix metalloproteinase secretion.

Entities: Disease Gene Species

Keywords: Embryo; Matrix Metalloproteinase (MMP); Mouse Genetics; Rab; Rab11; Rab11a; Trafficking; rab11

Mesh：

Substances：

Year: 2014 PMID： 25271168 PMCID： PMC4231680 DOI： 10.1074/jbc.M113.538223

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

76 in total

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