Post-Reconstitution Hemostatic Stability Profiles of Canadian and German Freeze-Dried Plasma

Henry T Peng; Katherine Moes; Kanwal Singh; Shawn G Rhind; Chantale Pambrun; Craig Jenkins; Luis da Luz; Andrew Beckett

doi:10.3390/life14020172

Post-Reconstitution Hemostatic Stability Profiles of Canadian and German Freeze-Dried Plasma

Life (Basel). 2024 Jan 24;14(2):172. doi: 10.3390/life14020172.

Authors

Henry T Peng¹, Katherine Moes¹, Kanwal Singh², Shawn G Rhind¹, Chantale Pambrun³, Craig Jenkins³, Luis da Luz⁴, Andrew Beckett^{2

5}

Affiliations

¹ Defence Research and Development Canada, Toronto Research Centre, Toronto, ON M3K 2C9, Canada.
² St. Michael's Hospital, University of Toronto, Toronto, ON M5B 1W8, Canada.
³ Centre for Innovation, Canadian Blood Services, Ottawa, ON K1G 4J5, Canada.
⁴ Sunnybrook Health Sciences Centre, University of Toronto, Toronto, ON M4N 3M5, Canada.
⁵ Royal Canadian Medical Services, Ottawa, ON K1A 0K2, Canada.

Abstract

Despite the importance of the hemostatic properties of reconstituted freeze-dried plasma (FDP) for trauma resuscitation, few studies have been conducted to determine its post-reconstitution hemostatic stability. This study aimed to assess the short- (≤24 h) and long-term (≥168 h) hemostatic stabilities of Canadian and German freeze-dried plasma (CFDP and LyoPlas) after reconstitution and storage under different conditions. Post-reconstitution hemostatic profiles were determined using rotational thromboelastometry (ROTEM) and a Stago analyzer, as both are widely used as standard methods for assessing the quality of plasma. When compared to the initial reconstituted CFDP, there were no changes in ROTEM measurements for INTEM maximum clot firmness (MCF), EXTEM clotting time (CT) and MCF, and Stago measurements for prothrombin time (PT), partial thromboplastin time (PTT), D-dimer concentration, plasminogen, and protein C activities after storage at 4 °C for 24 h and room temperature (RT) (22-25 °C) for 4 h. However, an increase in INTEM CT and decreases in fibrinogen concentration, factors V and VIII, and protein S activities were observed after storage at 4 °C for 24 h, while an increase in factor V and decreases in antithrombin and protein S activities were seen after storage at RT for 4 h. Evaluation of the long-term stability of reconstituted LyoPlas showed decreased stability in both global and specific hemostatic profiles with increasing storage temperatures, particularly at 35 °C, where progressive changes in CT and MCF, PT, PTT, fibrinogen concentration, factor V, antithrombin, protein C, and protein S activities were seen even after storage for 4 h. We confirmed the short-term stability of CFDP in global hemostatic properties after reconstitution and storage at RT, consistent with the shelf life of reconstituted LyoPlas. The long-term stability analyses suggest that the post-reconstitution hemostatic stability of FDP products would decrease over time with increasing storage temperature, with a significant loss of hemostatic functions at 35 °C compared to 22 °C or below. Therefore, the shelf life of reconstituted FDP should be recommended according to the storage temperature.

Keywords: coagulation; freeze-dried plasma; hemostatic resuscitation; prehospital transfusion; stability.

Grants and funding

People_014/Canadian Forces Health Services, the CF Surgeon Generals Health Research Program, and Defence Research and Development Canada