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Injectable Colloidal Hydrogels of -Vinylformamide Microgels Dispersed in Covalently Interlinked pH-Responsive Methacrylic Acid-Based Microgels. | LitMetric

AI Article Synopsis

  • Injectable hydrogels can help repair damaged soft tissues, and their stiffness should match that of the target tissue.
  • Traditional synthetic hydrogels have drawbacks, such as potential diffusion away from the injection site.
  • The study proposes a new injectable hydrogel made from modified microgels, allowing for better control over mechanical properties, making it a suitable option for spinal disk repair with lower cytotoxicity.

Article Abstract

Injectable hydrogels offer great potential to augment damaged or degenerated soft tissues. A key criterion for such gels is that their modulus is as close as possible to that of the target tissue. The majority of synthetic hydrogels have used low molecular weight polymer chains which may cause problems if they diffuse away from the injection site and/or increase the local osmotic pressure. We previously introduced a different approach of injecting preformed ultra-high molecular weight pH-responsive microgels (MGs) that interlink to form hydrogels. MGs are crosslinked polymer colloid particles that swell when the pH approaches the particle p. These colloidal hydrogels are termed doubly crosslinked microgels (DX MGs). The gel moduli of previous DX MGs were much greater than that reported for human nucleus pulposus (NP) tissue of the spinal intervertebral disk. Here, we replace some of the pH-responsive poly(ethyl acrylate--methacrylic acid) (PEA-MAA) MGs with hydrophilic non-ionic MGs based on poly(-vinylformamide) (NVF). We investigate the morphology and mechanical properties of these new injectable composite DX MGs and show that the mechanical properties can be tuned by systematically varying the NVF MG content. Using this approach, the gel moduli close to that for NP tissue are achieved. These injectable new pH-responsive gels exhibit low cytotoxicity. Our work provides a potential new system for minimally invasive intervertebral disk augmentation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10170504PMC
http://dx.doi.org/10.1021/acs.biomac.3c00058DOI Listing

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