4.8 Article

Optically Responsive Protein Coating of DNA Origami for Triggered Antigen Targeting

期刊

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acsami.2c10058

关键词

DNA nanotechnology; protein coating; photoresponsiveness; antigen targeting; electrostatic binding

资金

  1. European Research Council (ERC) under the European Union [101002258]
  2. Emil Aaltonen Foundation
  3. Sigrid Juslius Foundation
  4. Jane and Aatos Erkko Foundation
  5. VTT Technical Research Centre of Finland
  6. Academy of Finland Centers of Excellence Program [346110]
  7. Micronova Nano- fabrication Center
  8. European Research Council (ERC) [101002258] Funding Source: European Research Council (ERC)

向作者/读者索取更多资源

DNA nanostructures are susceptible to degradation, but coating them with proteins can protect and control their interaction with antigens through optical stimulation.
DNA nanostructures have emerged as modular building blocks in several research fields including biomedicine and nanofabrication. Their proneness to degradation in various environments has led to the development of a variety of nature-inspired protection strategies. Coating of DNA origami nanostructures with proteins can circumvent degradation and alter their properties. Here, we have used a single-chain variable antibody fragment and serum albumin to construct positively charged and stimuli-responsive proteindendron conjugates, which were complexed with DNA origami through electrostatic interactions. Using a stepwise assembly approach, the coated nanostructures were studied for their interaction with the corresponding antigen in fluorescence-based immunoassays. The results suggest that the antibody-antigen interaction can be disturbed by the addition of the bulky serum albumin. However, this effect is fully reversible upon irradiation of the structures with an optical stimulus. This leads to a selective dissociation of the serum albumin from the nanostructure due to cleavage of a photolabile group integrated in the dendron structure, exposing the antibody fragment and enabling triggered binding to the antigen, demonstrating that serum albumin can be considered as an externally controlled camouflaging agent. The presented stimuli-responsive complexation approach is highly versatile regarding the choice of protein components and could, therefore, find use in DNA origami protection, targeting, and delivery as well as their spatiotemporal control.

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