4.4 Article

Covalent Binding of BMP-2 on Surfaces Using a Self-assembled Monolayer Approach

Journal

JOVE-JOURNAL OF VISUALIZED EXPERIMENTS
Volume -, Issue 78, Pages -

Publisher

JOURNAL OF VISUALIZED EXPERIMENTS
DOI: 10.3791/50842

Keywords

Chemistry; Issue 78; Biochemistry; Chemical Engineering; Bioengineering; Biomedical Engineering; Biophysics; Genetics; Chemical Biology; Physical Chemistry; Proteins; life sciences; Biological Factors; Chemistry and Materials (General); Bone morphogenetic protein 2 (BMP-2); self-assembled monolayer (SAM); covalent immobilization; NHS-linker; BMP-2 signaling; protein; assay

Funding

  1. Max-Planck-Gesellschaft
  2. Deutsche Forschungsgemeinschaft (DFG) [SFB/TR79]

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Bone morphogenetic protein 2 (BMP-2) is a growth factor embedded in the extracellular matrix of bone tissue. BMP-2 acts as trigger of mesenchymal cell differentiation into osteoblasts, thus stimulating healing and de novo bone formation. The clinical use of recombinant human BMP-2 (rhBMP-2) in conjunction with scaffolds has raised recent controversies, based on the mode of presentation and the amount to be delivered. The protocol presented here provides a simple and efficient way to deliver BMP-2 for in vitro studies on cells. We describe how to form a self-assembled monolayer consisting of a heterobifunctional linker, and show the subsequent binding step to obtain covalent immobilization of rhBMP-2. With this approach it is possible to achieve a sustained presentation of BMP-2 while maintaining the biological activity of the protein. In fact, the surface immobilization of BMP-2 allows targeted investigations by preventing unspecific adsorption, while reducing the amount of growth factor and, most notably, hindering uncontrolled release from the surface. Both short-and long-term signaling events triggered by BMP-2 are taking place when cells are exposed to surfaces presenting covalently immobilized rhBMP-2, making this approach suitable for in vitro studies on cell responses to BMP-2 stimulation.

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