Use of clinical data and acceleration profiles to validate pneumatic transportation systems

Author:

Gils Charlotte12,Broell Franziska3,Vinholt Pernille J.12,Nielsen Christian4,Nybo Mads25

Affiliation:

1. Department of Clinical Biochemistry and Pharmacology , Odense University Hospital , Odense C , Denmark

2. Clinical Institute , University of Southern Denmark , Odense , Denmark

3. Motryx Inc. , Halifax , Canada

4. Department of Clinical Immunology , Odense University Hospital , Odense , Denmark

5. Department of Clinical Diagnostics , Hospital of South West Jutland , Esbjerg , Denmark

Abstract

Abstract Background Modern pneumatic transportation systems (PTSs) are widely used in hospitals for rapid blood sample transportation. The use of PTS may affect sample integrity. Impact on sample integrity in relation to hemolysis and platelet assays was investigated and also, we wish to outline a process-based and outcome-based validation model for this preanalytical component. Methods The effect of PTS was evaluated by drawing duplicate blood samples from healthy volunteers, one sent by PTS and the other transported manually to the core laboratory. Markers of hemolysis (potassium, lactate dehydrogenase [LD] and hemolysis index [HI]) and platelet function and activation were assessed. Historic laboratory test results of hemolysis markers measured before and after implementation of PTS were compared. Furthermore, acceleration profiles during PTS and manual transportation were obtained from a mini g logger in a sample tube. Results Hand-carried samples experienced a maximum peak acceleration of 5 g, while peaks at almost 15 g were observed for PTS. No differences were detected in results of potassium, LD, platelet function and activation between PTS and manual transport. Using past laboratory data, differences in potassium and LD significantly differed before and after PTS installation for all three lines evaluated. However, these estimated differences were not clinically significant. Conclusions In this study, we found no evidence of PTS-induced hemolysis or impact on platelet function or activation assays. Further, we did not find any clinically significant changes indicating an acceleration-dependent impact on blood sample quality. Quality assurance of PTS can be performed by surveilling outcome markers such as HI, potassium and LD.

Publisher

Walter de Gruyter GmbH

Subject

Biochemistry (medical),Clinical Biochemistry,General Medicine

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