What question did this study set out to answer?

The study aims to validate the efficacy of an anticoagulant-free method for preparing autologous f-PRF using a soft-spin centrifuge.

March 7, 2026Open Access

Anticoagulant-free preparation of autologous platelet-rich plasma (PRP) / fluid platelet-rich fibrin (f-PRF): a pre-clinical comparative performance study

Key Points

The study aims to validate the efficacy of an anticoagulant-free method for preparing autologous f-PRF using a soft-spin centrifuge.
Blood was collected from sixteen healthy volunteers for analysis.
f-PRF was prepared using the Exprecell™ and Arthrex ACP® systems through standardized centrifugation.
Cellular composition, platelet function, and growth factors were characterized after preparation.
Exprecell™ produced 20% more f-PRF volume compared to Arthrex ACP® (6.5–10.5 mL vs. 5.5–9.0 mL).
Over 99% erythrocyte and over 95% leukocyte reductions were achieved with Exprecell™.
Platelet counts and function were similar between the two systems, with maintained in vitro responses.

Abstract

Objective This study aimed to validate and characterize the efficacy of a previously developed anticoagulant-free, single soft-spin centrifugation device for the preparation of autologous fluid-Platelet-Rich Fibrin (f-PRF). Introduction f-PRF is generated via one-step soft-spin centrifugation of all blood to produce a platelet-enriched plasma for regenerative medicine use, without the need for additional chemical agents. This study validated the performance of a novel single soft-spin f-PRF preparation system. Methods Sixteen healthy volunteers (94% female, ages 23-52) donated blood for a comparative analysis between Exprecell™ and Arthrex ACP ® Double-Syringe systems. f-PRF was prepared using standardized centrifugation (420 xg , 5 min) and characterized for cellular composition, platelet function, growth factors, and extracellular vesicles (EVs). Platelet activation was assessed via P-selectin expression and GPIIb/IIIa activation following stimulation using flow cytometry. Results Exprecell™ yielded 20% more f-PRF volume (6.5–10.5 vs. 5.5–9.0 mL) with excellent cellular depletion (99% erythrocyte, 95% leukocyte reduction). Platelet counts and function were similar between systems, with preserved in vitro agonist responses in terms of P-selectin expression and GPIIb/IIIa activation. Most growth factors remained below detection limits, and those detectable showed no differences between the devices. EV profiles from different cell types were also comparable. Conclusion These findings support the Exprecell™ single soft-spin methodology, demonstrating that anticoagulant-free f-PRF preparation achieves functional equivalence to conventional methods while providing a statistically significant increase in volume yield and procedural simplicity. The closed system design reduces contamination risk and Luer-lock compatibility facilitates integration into clinical workflows. Maintained in vitro biological activity supports clinical utility for this innovative point-of-care f-PRF preparation device. Future studies are needed to demonstrate the clinical benefit of the f-PRF obtained.

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Cite This Study

Assinger et al. (Wed,) studied this question.

synapsesocial.com/papers/69abc1015af8044f7a4e9ac6 https://doi.org/https://doi.org/10.3389/fphar.2026.1785884

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