4.7 Article

Network confinement and heterogeneity slows nanoparticle diffusion in polymer gels

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JOURNAL OF CHEMICAL PHYSICS
卷 146, 期 20, 页码 -

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AMER INST PHYSICS
DOI: 10.1063/1.4978054

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资金

  1. NSF [PIRE OISE-1545884, ACS/PRF 54028-ND7, NSF/MWN DMR-1210379, NSF/DMR 1507713]
  2. National Institute of Health via an Interdisciplinary Cardiovascular Training Grant [5T32HL007954-15]
  3. Nano Bio Interface Center (NBIC) at the University of Pennsylvania through NSF [NSEC DMR08-32802, MRI DBI-0721913]
  4. Direct For Mathematical & Physical Scien
  5. Division Of Materials Research [1507713] Funding Source: National Science Foundation

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Nanoparticle (NP) diffusion was measured in polyacrylamide gels (PAGs) with a mesh size comparable to the NP size, 21 nm. The confinement ratio (CR), NP diameter/mesh size, increased from 0.4 to 3.8 by increasing crosslinker density and from 0.4 to 2.1 by adding acetone, which collapsed the PAGs. In all gels, NPs either became localized, moving less than 200 nm, diffused microns, or exhibited a combination of these behaviors, as measured by single particle tracking. Mean squared displacements (MSDs) of mobile NPs decreased as CR increased. In collapsed gels, the localized NP population increased and MSD of mobile NPs decreased compared to crosslinked PAGs. For all CRs, van Hove distributions exhibited non-Gaussian displacements, consistent with intermittent localization of NPs. The non-Gaussian parameter increased from a maximum of 1.5 for crosslinked PAG to 5 for collapsed PAG, consistent with greater network heterogeneity in these gels. Diffusion coefficients decreased exponentially as CR increased for crosslinked gels; however, in collapsed gels, the diffusion coefficients decreased more strongly, which was attributed to network heterogeneity. Collapsing the gel resulted in an increasingly tortuous pathway for NPs, slowing diffusion at a given CR. Understanding how gel structure affects NP mobility will allow the design and enhanced performance of gels that separate and release molecules in membranes and drug delivery platforms. Published by AIP Publishing.

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