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Protein-Nanoparticle Interactions Govern the Interfacial Behavior of Polymeric Nanogels: Study of Protein Corona Formation at the Air/Water Interface. | LitMetric

AI Article Synopsis

  • Understanding how nanoparticles interact with biological systems is crucial for their biomedical applications, as the formation of a protein corona can change the nanoparticles' characteristics.
  • This study investigates how acrylamide-based nanogels with different charges interact with important proteins found in serum, using techniques like dynamic light scattering and neutron reflectometry to analyze these interactions.
  • The findings highlight that the structure of proteins at the interface affects the nanomaterials' properties, providing insights that could enhance drug delivery systems.

Article Abstract

Biomedical applications of nanoparticles require a fundamental understanding of their interactions and behavior with biological interfaces. Protein corona formation can alter the morphology and properties of nanomaterials, and knowledge of the interfacial behavior of the complexes, using in situ analytical techniques, will impact the development of nanocarriers to maximize uptake and permeability at cellular interfaces. In this study we evaluate the interactions of acrylamide-based nanogels, with neutral, positive, and negative charges, with serum-abundant proteins albumin, fibrinogen, and immunoglobulin G. The formation of a protein corona complex between positively charged nanoparticles and albumin is characterized by dynamic light scattering, circular dichroism, and surface tensiometry; we use neutron reflectometry to resolve the complex structure at the air/water interface and demonstrate the effect of increased protein concentration on the interface. Surface tensiometry data suggest that the structure of the proteins can impact the interfacial properties of the complex formed. These results contribute to the understanding of the factors that influence the bio-nano interface, which will help to design nanomaterials with improved properties for applications in drug delivery.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9917661PMC
http://dx.doi.org/10.3390/ijms24032810DOI Listing

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