4.7 Article

Simultaneous Cross-Linking and Cross-Polymerization of Enzyme Responsive Polyethylene Glycol Nanogels in Confined Aqueous Droplets for Reduction of Low-Density Lipoprotein Oxidation

Journal

BIOMACROMOLECULES
Volume 22, Issue 2, Pages 386-398

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.biomac.0c01238

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Funding

  1. Lundbeck Fellowship [R215-2015-4190]
  2. Technical University of Denmark, Department of Health Technology

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This study focuses on the initiating mechanism of atherosclerosis and presents the development of therapeutic nanogels using biocompatible PEG cross-linking method. The nanogels release anti-inflammatory and anti-oxidizing enzyme PON-1 to reduce the production of ox-LDL, effectively inhibiting macrophage foam cell and reactive oxygen species formation.
A key initiating step in atherosclerosis is the accumulation and retention of apolipoprotein B complexing lipoproteins within the artery walls. In this work, we address this exact initiating mechanism of atherosclerosis, which results from the oxidation of low-density lipoproteins (oxLDL) using therapeutic nanogels. We present the development of biocompatible polyethylene glycol (PEG) cross-linked nanogels formed from a single simultaneous cross-linking and co-polymerization step in water without the requirement for an organic solvent, high temperature, or shear stress. The nanogel synthesis also incorporates in situ noncovalent electrostatically driven template polymerization around an innate anti- inflammatory and anti-oxidizing paraoxonase-1 (PON-1) enzyme payload-the release of which is triggered because of matrix metalloproteinase responsive elements instilled in the PEG cross-linker monomer. The results obtained demonstrate the potential of triggered release of the PON-1 enzyme and its efficacy against the production of ox-LDL, and therefore a reduction in macrophage foam cell and reactive oxygen species formation.

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