Description

The chemokine, stromal cell-derived factor 1α (SDF-1α), is a key regulator of the endogenous neural progenitor/stem cell-mediated regenerative response after neural injury. Increased and sustained bioavailability of SDF-1α in the peri-injury region is hypothesized to modulate this endogenous repair response.

The chemokine, stromal cell-derived factor 1α (SDF-1α), is a key regulator of the endogenous neural progenitor/stem cell-mediated regenerative response after neural injury. Increased and sustained bioavailability of SDF-1α in the peri-injury region is hypothesized to modulate this endogenous repair response. Here, we describe poly(lactic-co-glycolic) acid (PLGA) nanoparticles capable of releasing bioactive SDF-1α in a sustained manner over 60 days after a burst of 23%. Moreover, we report a biphasic cellular response to SDF-1α concentrations thus the large initial burst release in an in vivo setting may result in supratherapeutic concentrations of SDF-1α. Specific protein–protein interactions between SDF-1α and fibrin (as well as its monomer, fibrinogen) were exploited to control the magnitude of the burst release. Nanoparticles embedded in fibrin significantly reduced the amount of SDF-1α released after 72 h as a function of fibrin density. Therefore, the nanoparticle/fibrin composites represented a means to independently tune the magnitude of the burst phase release from the nanoparticles while perserving a bioactive depot of SDF-1α for release over 60 days.

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  • Details

    Title
    • Tunable Controlled Release of Bioactive SDF-1α Via Specific Protein Interactions Within Fibrin/Nanoparticle Composites
    Contributors
    Date Created
    2015-08-11
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    Identifier
    • Digital object identifier: 10.1039/C5TB00935A
    • Identifier Type
      International standard serial number
      Identifier Value
      2050-750X

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    Dutta, D., Fauer, C., Mulleneux, H. L., & Stabenfeldt, S. E. (2015). Tunable controlled release of bioactive SDF-1α via specific protein interactions within fibrin/nanoparticle composites. Journal of Materials Chemistry B, 3(40), 7963-7973. DOI: 10.1039/C5TB00935A

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