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Thromb Haemost 1973; 30(02): 393-402
DOI: 10.1055/s-0038-1649089
Original Article
Schattauer GmbH

Studies on Activator Formation in Human Plasma with Streptokinase

II. Quantitative Activator and Plasminogen Measurements during Continuous and Intermittent Streptokinase Infusion
M Martin
1   Medizinische Universitäts-Poliklinik Bonn and the Aggertalklinik Engelskirchen bei Köln
,
with the technical assistance of Frau R. Albrecht › Institutsangaben
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Publikationsverlauf

Received for publication 08. Dezember 1972

Accepted for publication 17. Mai 1973

Publikationsdatum:
24. Juli 2018 (online)

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Summary

The activator concentrations developing during a streptokinase infusion treatment were measured on a quantitative basis. The reference value (100 per cent activator) selected for this purpose was the activator effectiveness resulting from a mixture of 20,000 units of streptokinase and 1 millilitre of citrate plasma. The streptokinase treatment regimens used for our study consisted either of a continuous streptokinase infusion treatment extended over three days or of intermittent streptokinase infusions with a 16-hour streptokinase-free interval. The highest activator concentrations measured had developed between 1 and 24 hours after the streptokinase treatment had started, the values being in the order of 0.4 per cent. When treatment was continued, the activator concentrations dropped below that level. Under the intermittent streptokinase regimen, the activator concentrations measured during the second series of infusions were always lower than those measured during the first series. The activator concentration levels and the plasminogen values measured simultaneously acted in a reciprocal manner, i.e. a plasminogen decrease corresponded to an activator increase and vice versa. Seen under the aspect of the obtainable maximum of activator effectiveness, the intermittent streptokinase infusion regimen offers no advantage as against the continuous treatment form. It would certainly be desirable to achieve higher activator levels through modifications in the streptokinase dosage.

 

  • References

  • 1 Amery A. 1967. Diskussionsbeitrag. In: Hess H. (ed.) Thrombolytische Therapie. Symposion der Deutschen Gesellschaft für Angiologie. 4. Jahrestagung 1966. F. K. Schattauer-Verlag; Stuttgart: 22.
    Suche in Google Scholar
  • 2 Amery A. 1969. Changes in fibrinolytic parameters after prolonged streptokinase infusion. In: Hiemeyee V. (ed.) Therapeutische und experimentelle Fibrinolyse. F. K. Schattauer-Verlag; Stuttgart-New York.: 151.
    Suche in Google Scholar
  • 3 Blix S. 1964; The proactivator (plasminogen) determination in plasma during fibrinolytic therapy. Acta medica scandinavica 176: 649.
    PubMedSuche in Google Scholar
  • 4 Blix S. 1969; The activater time. A method for control of activator activity during thrombolytic therapy. Scandinavian Journal of Haematology 6: 221.
    PubMedSuche in Google Scholar
  • 5 Davies M. C, Englebeet M. E, and de Renzo E. C. 1964; Interaction of streptokinase and human plasminogen. I. Combining of streptokinase and plasminogen observed in the ultracentri- fuge under a variety of experimental conditions. Journal of Biological Chemistry 239: 2651.
    PubMedSuche in Google Scholar
  • 6 Deutsch E, Denk H, and Fischer M. 1969; Derzeitiger Stand und Aussichten der thrombo- lytischen Therapie. Wiener medizinische Wochenschrift 119: 85.
    PubMedSuche in Google Scholar
  • 7 Deutsch E, and Fischer M. 1960; Die Wirkung intravenös applizierter Streptokinase auf Fibrinolyse und Blutgerinnung. Thrombosis et Diathesis Haemorrhagica 6: 482.
    PubMedSuche in Google Scholar
  • 8 Fletcher A. P, Alkjaersig N, and Sherry S. 1958; The clearance of heterologous protein from the circulation of normal and immunized man. Journal of Clinical Investigation 37: 1306.
    CrossrefPubMedSuche in Google Scholar
  • 9 Hiemeyer V, and Rasche H. 1966; Der Mechanismus der Streptokinaseinduzierten Thrombolyse und seine Bedeutung für die Therapie akuter Gefäßverschlüsse. Klinische Wochenschrift 44: 539.
    CrossrefPubMedSuche in Google Scholar
  • 10 Hirsh J, Hale G. S, McDonald McCarthy R. A, and Cade F. J. 1967; Resolution of acute massive pulmonary embolism after pulmonary arterial infusion of streptokinase. Lancet II: 593.
    PubMedSuche in Google Scholar
  • 11 Hummel B. C. W, Buck F. F, and de Renzo E. C. 1966; Interaction of streptokinase and human plasminogen. Journal of Biological Chemistry 241: 3474.
    PubMedSuche in Google Scholar
  • 12 Martin Martin M. 1969; Semiquantitative Plasminogenbestimmung mit Hilfe des Thrombelasto-graphen. Eine Methode zur Kontrolle der Streptokinasebehandlung. Thrombosis et Diatehesis Haemorrhagica 22: 121.
    PubMedSuche in Google Scholar
  • 13 Martin M. 1973; Studies on activator formation. I. Experimental studies. Thrombosis et Diathesis Haemorrhagica 30: 381.
    PubMedSuche in Google Scholar
  • 14 Poliwoda H. 1969. Zur Dosierung von Streptokinase. In: Hiemeyer V. (ed.) Therapeutische und experimentelle Fibrinolyse. Internationales Symposion vom 29. Sept. bis 1. Okt. 1967 in Ulm (Donau). F. K. Schattauer-Verlag; Stuttgart-New York: 147.
    Suche in Google Scholar
  • 15 Rasche H, Hiemeyer V, and Heimpel H. 1969. Verteilungsstudien mit radioaktiv markierter Streptokinase. In: Hiemeyer V. (ed.) Therapeutische und experimentelle Fibrinolyse. Internationales Symposion 1967. F. K. Schattauer-Verlag; Stuttgart-New York.: 133.
    Suche in Google Scholar
  • 16 de Renzo E. C. 1961; Chemistry of fibrinolysis. (Discussion): Thrombosis et Diathesis Haemorrhagica Suppl. 1 ad 6: 134.
    PubMedSuche in Google Scholar
  • 17 Verstraete M, Amery A, Vermylen J, Vermylen C, and de Vreker R. 1964; Practical method for thrombolytic therapy with streptokinase. Maintenance of nearly complete plasminogen depletion associated with high circulating activator activity. British Medical Journal 1: 675.
    CrossrefPubMedSuche in Google Scholar