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Time-resolved serial femtosecond crystallography for investigating structural dynamics of chemical systems.

Jungho MoonYunbeom LeeHyotcherl Ihee
Published in: Chemical communications (Cambridge, England) (2024)
Time-resolved serial femtosecond crystallography (TR-SFX) has emerged as a crucial tool for studying the structural dynamics of proteins. In principle, TR-SFX has the potential to be a powerful tool not only for studying proteins but also for investigating chemical reactions. However, non-protein systems generally face challenges in indexing due to sparse Bragg spots and encounter difficulties in effectively exciting target molecules. Nevertheless, successful TR-SFX studies on chemical systems have been recently reported in a few instances, boding well for the application of TR-SFX to study chemical reactions in the future. In this context, we review the static SFX and TR-SFX studies conducted on chemical systems reported to date and suggest prospects for future research directions.
Keyphrases
  • current status
  • small molecule
  • neural network