ID | 113586 |
Title Alternative | Ameloblastin regulates osteogenic differentiation by inhibiting Src kinase via crosstalk between integrin β1 and CD63
Ameloblastin regulates osteogenic differentiation
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Author |
Iizuka, Shinji
Hiroshima University
Kudo, Yasusei
Hiroshima University
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Yoshida, Maki
Hiroshima University
Tsunematsu, Takaaki
Hiroshima University
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Yoshiko, Yuji
Hiroshima University
Uchida, Takashi
Hiroshima University
Ogawa, Ikuko
Hiroshima University
Miyauchi, Mutsumi
Hiroshima University
Takata, Takashi
Hiroshima University
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Content Type |
Journal Article
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Description | Ameloblastin, the most abundant non-amelogenin enamel matrix protein, plays a role in ameloblast differentiation. Here we found that ameloblastin was expressed in osteosarcoma cells; to explore the potential functions of ameloblastin in osteoblasts, we investigated whether this protein is involved in osteogenic differentiation and bone formation on the premise that CD63, a member of the transmembrane-4 glycoprotein superfamily, interacts with integrins in the presence of ameloblastin. Ameloblastin bound to CD63 and promoted CD63 binding to integrin β1. The interaction between CD63 and integrin β1 induced Src kinase inactivation via the binding of CD63 to Src. The reduction of Src activity and osteogenic differentiation mediated by ameloblastin was abrogated by treatment with anti-CD63 antibody and overexpression of constitutive active Src, respectively. Moreover, amelobastin upregulated the formation of stress-fibre and focal adhesions and downregulated cell migration in association with RhoA regulation via Src activity. Therefore, our results suggest that ameloblastin is expressed in osteoblasts and functions as a promoting factor for osteogenic differentiation via a novel pathway through the interaction between CD63 and integrin β1.
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Journal Title |
Molecular and Cellular Biology
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ISSN | 02707306
10985549
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NCID | AA10620925
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Publisher | American Society for Microbiology
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Volume | 31
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Issue | 4
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Start Page | 783
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End Page | 792
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Published Date | 2011-01-26
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EDB ID | |
DOI (Published Version) | |
URL ( Publisher's Version ) | |
FullText File | |
language |
eng
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TextVersion |
Author
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departments |
Oral Sciences
Medical Sciences
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