4.8 Article

Conformational Details of Quantum Dot-DNA Resolved by Forster Resonance Energy Transfer Lifetime Nanoruler

期刊

ACS NANO
卷 13, 期 1, 页码 505-514

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acsnano.8b07137

关键词

FRET; quantum dots; nanoparticles; terbium; molecular ruler; conformation; sensing

资金

  1. European Commission (H2020-FET-Open project PROSEQO)
  2. French National Research Agency (ANR)
  3. China Scholarship Council (CSC)
  4. ONR
  5. NRL
  6. NRL-Nanosciences Institute
  7. LUCI grant
  8. Institut Universitaire de France (IUF)

向作者/读者索取更多资源

DNA-nanoparticle conjugates are important tools in nanobiotechnology. Knowing the orientation, function, and length of DNA on nanoparticle surfaces at low nanomolar concentrations under physiological conditions is therefore of great interest. Here, we investigate the conformation of a 31 nucleotides (nt) long DNA attached to a semiconductor quantum dot (QD) via Forster resonance energy transfer (FRET) from Tb-DNA probes hybridized to different positions on the QD-DNA. Precise Tb-to-QD distance determination from 7 to 14 nm along 26 nt of the peptide-appended QD-DNA was realized by time-resolved FRET spectroscopy. The FRET nanoruler measured linear single-stranded (ssDNA) and double-stranded (dsDNA) extensions of similar to 0.15 and similar to 0.31 nm per base, reflecting the different conformations. Comparison with biomolecular modeling confirmed the denser conformation of ssDNA and a possibly more flexible orientation on the QD surface, whereas the dsDNA was fully extended with radial orientation. The temporally distinct photoluminescence decays of the different DNA-FRET configurations were used for prototypical DNA hybridization assays that demonstrated the large potential for extended temporal multiplexing. The extensive experimental and theoretical analysis of 11 different distances/configurations of the same QD-DNA conjugate provided important information on DNA conformation on nanoparticle surfaces and will be an important benchmark for the development and optimization of DNA-nanobiosensors.

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