研究目的
To review and analyze sample delivery methods for serial femtosecond crystallography at X-ray free-electron lasers, aiming to facilitate high-throughput and automated experiments for structural biology.
研究成果
SFX enables room-temperature, damage-free structure determination of macromolecules using X-ray FELs. High repetition rates promise reduced measurement times and sample consumption, but require advanced, automated sample delivery systems. A universal, robotic-based setup with feedback control is proposed to enhance throughput, reliability, and flexibility for diverse experimental needs, facilitating broader applications in structural biology.
研究不足
Current sample delivery systems are not fully optimized for high repetition rate FELs like the European XFEL, requiring speeds over 450 m/s. Issues include jet instability, clogging, high sample consumption, and background from carrying media. Manual interventions and alignment drifts lead to downtime, and not all methods are transferable to future facilities without modifications.
1:Experimental Design and Method Selection:
The paper reviews existing sample delivery technologies for SFX, including in-air goniometers, in-vacuum sample arrays, aerosol particle injectors, gas-focused liquid jets, electrospun jets, and extruded viscous flows. It discusses their suitability based on FEL pulse rates and sample properties.
2:Sample Selection and Data Sources:
Focuses on protein crystals and other biological samples, with data from experiments at facilities like LCLS and SACLA.
3:List of Experimental Equipment and Materials:
Includes various nozzles, injectors, detectors (e.g., CSPAD, MPCCD, AGIPD), and sample delivery systems such as GDVNs and LCP extrusion nozzles.
4:Experimental Procedures and Operational Workflow:
Describes the setup for delivering samples to the X-ray beam, including jet formation, alignment, and data collection processes. Proposes an automated system with robotic handling and feedback control.
5:Data Analysis Methods:
Mentions the Monte Carlo integration method for processing diffraction patterns to obtain structure factors, with metrics like Rsplit for data quality assessment.
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