4.8 Article

Resolving Single-Nanoconstruct Dynamics during Targeting and Nontargeting Live-Cell Membrane Interactions

Journal

ACS NANO
Volume 13, Issue 12, Pages 13637-13644

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsnano.9b03144

Keywords

differential interference contrast microscopy; singleparticle dynamics; targeting and nontargeting nanoconstructs; protein corona; membrane-receptor interactions

Funding

  1. NIH [R01GM115763]
  2. NASA Ames Research Center [NNA06CB93G]
  3. NCI CCSG [P30 CA060553]
  4. [P41 GM108569]

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This paper describes how differences in the dynamics of targeting and nontargeting constructs can provide information on nanoparticle (NP)-cell interactions. We probed translational and rotational dynamics of functionalized Au nanostar (AuNS) nanoconstructs interacting with cells in serum-containing medium. We found that AuNS with targeting ligands had a larger dynamical footprint and faster rotational speed on cell membranes expressing human epidermal growth factor receptor 2 (HER-2) receptors compared to that of AuNS with nontargeting ligands. Targeting and nontargeting nano constructs displayed distinct membrane dynamics despite their similar protein adsorption profiles, which suggests targeted interactions are preserved even in the presence of a protein corona. The high sensitivity of single-NP dynamics can be used to compare different nanoconstruct properties (such as NP size, shape, and surface chemistry) to improve their design as delivery vehicles.

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