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Cell adhesion to anosmin via α5β1, α4β1, and α9β1 integrins.

Cell adhesion & migration (2016-10-08)
Yukinori Endo, Hiroko Ishiwata-Endo, Kenneth M Yamada
ZUSAMMENFASSUNG

Anosmin is an extracellular matrix protein, and genetic defects in anosmin result in human Kallmann syndrome. It functions in neural crest formation, cell adhesion, and neuronal migration. Anosmin consists of multiple domains, and it has been reported to bind heparan sulfate, FGF receptor, and UPA. In this study, we establish cell adhesion/spreading assays for anosmin and use them for antibody inhibition analyses to search for an integrin adhesion receptor. We find that α5β1, α4β1, and α9β1 integrins are needed for effective adhesive receptor function in cell adhesion and cell spreading on anosmin; adhesion is inhibited by both RGD and α4β1 CS1-based peptides. This identification of anosmin-integrin adhesion receptors should facilitate studies of anosmin function in cell and developmental biology.

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Anti-Integrin αVβ3 Antibody, clone LM609, clone LM609, Chemicon®, from mouse
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Anti-Integrin α1 Antibody, clone FB12, clone FB12, Chemicon®, from mouse
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Anti-Integrin α2 Antibody, clone P1E6, clone P1E6, Chemicon®, from mouse
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Anti-Integrin α4 Antibody, clone P1H4, clone P1H4, Chemicon®, from mouse
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Anti-Integrin β4 Antibody, clone ASC-9, clone ASC-9, Chemicon®, from mouse
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Anti-Integrin β2 Antibody, clone P4H9, clone P4H9, Chemicon®, from mouse