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DOI: 10.1055/s-0038-1649130
Controlled-flow Instruments for Simulating in Vivo Thrombosis
Publication History
Received
20 July 1973
Accepted
14 August 1973
Publication Date:
30 June 2018 (online)
Summary
A technique has been developed which allows an estimation of the clotting tendency of blood under conditions which simulate in vivo flow in various regions of the circulatory system. Minimum contact between blood and foreign surfaces other than the walls of the tubular test cell is obtained. Early pre-clotting and clotting events which alter the apparent viscosity of blood are resolved within three seconds of their onset. Increases in apparent viscosity slow the oscillations of the test system, and frequency, differential frequency, or amplitude can be monitored continuously. A standard tubing material may be used to evaluate effects of antithrombotic or other agents. For the present studies, the instrument was used with native blood at 28° or 37° C to produce shear rates comparable to those present in venous flow. Gum rubber, vinyl, glass and silicone tubing have been investigated for their effects on activation of the intrinsic coagulation system of human blood. In order of increasing-time to formation of thrombus are glass, vinyl, rubber, silicone. Thrombi were adherent to glass and rubber but not to Tygon or Silastic tubes. Time sequence studies during flow in silicone tube with native blood indicate progressive shortening of Stypven and partial thromboplastin time values, and progressive decrease in leukocyte and platelet counts. Addition of a commercial bovine collagen preparation to native normal blood in Silicone tubing decreased the thrombus time value by 40% while addition of the experimental agents RA 233 or VK 744 decreased this value by 50% and 70% respectively. Aspirin therapy produced a 158% increase in thrombus time values. Light microscopic studies of thrombi formed in this closed system revealed thrombus structure comparable to that of classic venous thrombi.
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References
- 1 Chandler A. B. 1958; In vitro Thrombotic Coagulation of Blood. A method of producing a thrombus. Laboratory Investigation 1: 110.
- 2 Dintenfass L. 1969; A Coaxial Rhombospheroid Viscometer: A Further Development of the Cone-in-cone Viscometer. Biorheology 6: 33.
- 3 Gott V. L, Whiffen J. D, and Dtttton R. C. 1963; Heparin Bonding on Colloidal Graphite Surfaces. Science 142: 1297.
- 4 Gott V. L, Ameli M. M, Whiffen J. D, Leininger R. I, and Falb R. D. 1967; Newer Thromboresistant Surfaces: Evaluation with a new in-vivo technique. Surgical Clinics of North America 47: 1443.
- 5 Hartert H. 1949; Blutgerinnungsstudien mit der Thrombelastographie, einem neuen Untersuchungsverfahren. Klinische Wochen-Schrift 27: 789.
- 6 Helmholtz H. V, and Piotrowski G. 1860; Sitzungsberichte der Akademie Wissenschaften. Wien 40: 607.
- 7 Miale J. B. 1962. Laboratory Medicine – Hematology. 2nd edition.. C. V. Mosby Co.; St. Louis: 1202.
- 8 Miescher P. A, and Gerarde H. W. 1966; A one-step method for counting leucocytes and platelets. American Journal of Clinical Pathology 46: 576.
- 9 Nye S. W, Graham J. B, and Brinkhous K. M. 1962; The partial thromboplastin time as a screening test for the detection of latent bleeders. American Journal of Medical Science 243: 279.
- 10 Virchow R. 1856. Gesammelte Abhandlungen zur wissenschaftlichen Medizin. Meidinge Sohn und Comp.; Frankfurt:
- 11 Whiffen J. D, Lightfoot E. N, Dennis W. H, Safford R. E, Powaser M. M, and Solen K. A. 1971; A Device to Study the Degradation of Blood in a Shear Field with Controlled Wall Effects. Journal of Biomedical Materials Research 5: 315.