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Comparison of surface plasmon resonance and quartz crystal microbalance in the study of whole blood and plasma coagulation

Year: 2000

Journal: BIOSENSORS & BIOELECTRONICS 15: (11-12) 605-613 DEC 2000, 20100827

Authors: Vikinge TP, Hansson KM, Sandstrom P, Liedberg B, Lindahl TL, Lundstrom I, Tengvall P, Hook F

Last authors: Hook F

Organizations: Linkoping Univ, IFM, Appl Phys Lab, S-58183 Linkoping, Sweden Linkoping Univ Hosp, Dept Biomed & Surg, Div Clin Chem, S-58185 Linkoping, Sweden Linkoping Univ, Forum Scientum Grad Sch, S-58183 Linkoping, Sweden Goteborg Grad Sch Biomed, S-41296 Gothenburg, Sweden Chalmers Univ Technol, Dept Appl Phys, S-41296 Gothenburg, Sweden Lundberg Inst, Dept Cell & Mol Biol, S-41390 Gothenburg, Sweden

Country: Sweden

The coagulation of blood plasma and whole blood was studied with a surface plasmon resonance (SPR) based device and a quartz crystal microbalance instrument with energy dissipation detection (QCM-D). The SPR and QCM-D response signals were similar in shape but differing in time scales, reflecting differences in detection mechanisms. The QCM-D response time was longer than SPR, as a physical coupling of the sample to the substrate is required for molecules to be detected by the QCM-method. Change of sample properties within the evanescent field is sufficient for detection with SPR. Both the SPR signals and the QCM-D frequency and dissipation shifts showed dependency on concentrations of coagulation activator and sensitivity to heparin additions. The ratio of dissipation to frequency shifts, commonly considered to reflect viscoelastic properties of the sample, varied with the concentration of activator in blood plasma but not in whole blood. Additions of heparin to the thromboplastin activated whole blood sample, however, made the ratio variation reoccur. Implications of these observations for the understanding of the blood coagulation processes as well as the potential of the two methods in the clinic and in research are discussed.