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Spatiotemporally controlled generation of NTPs for single-molecule studies.

Anton SabantsevGuanzhong MaoJavier Aguirre RiveraMikhail PanfilovAnatolii ArsenievOanh HoMikhail KhodorkovskiySebastian Deindl
Published in: Nature chemical biology (2022)
Many essential processes in the cell depend on proteins that use nucleoside triphosphates (NTPs). Methods that directly monitor the often-complex dynamics of these proteins at the single-molecule level have helped to uncover their mechanisms of action. However, the measurement throughput is typically limited for NTP-utilizing reactions, and the quantitative dissection of complex dynamics over multiple sequential turnovers remains challenging. Here we present a method for controlling NTP-driven reactions in single-molecule experiments via the local generation of NTPs (LAGOON) that markedly increases the measurement throughput and enables single-turnover observations. We demonstrate the effectiveness of LAGOON in single-molecule fluorescence and force spectroscopy assays by monitoring DNA unwinding, nucleosome sliding and RNA polymerase elongation. LAGOON can be readily integrated with many single-molecule techniques, and we anticipate that it will facilitate studies of a wide range of crucial NTP-driven processes.
Keyphrases
  • single molecule
  • living cells
  • atomic force microscopy
  • single cell
  • high resolution
  • high throughput
  • mass spectrometry
  • bone mineral density
  • body composition