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DOI: 10.1160/TH05-02-0123
The effect of long term, low-dose tranexamic acid treatment on platelet dysfunction and haemoglobin levels in haemodialysis patients
Publication History
Received
20 February 2005
Accepted after resubmission
05 September 2005
Publication Date:
07 December 2017 (online)
Summary
Some previous studies suggest that activation of the fibrinolytic system may induce platelet dysfunction in haemodialysis patients. Accordingly, inhibition of fibrinolysis may improve platelet dysfunction, and speculatively increase haemoglobin levels. We tested this hypothesis. The study group comprised 22 patients (14 male, 8 female, median age 62), who had been on maintenance haemodialysis for more than one year. Patients were treated for three months with low-dose tranexamic acid (TXA), a potent anti-fibrinolytic agent. The dosages of erythropoietin and the haemodialysis procedure were not changed significantly during the study. We primarily followed platelet function (by in vitro closure time test) and haemoglobin values. Patients were divided into those with substantially prolonged (N=9) and those with slightly delayed or normal (N=13) in vitro closure time. Treatment with TXA resulted in a significant improvement of platelet function and increased levels of haemoglobin in the first group, and no changes in either platelet function or haemoglobin values in the second group. TXA in the dosage used was biologically active, since a significant decrease in plasminogen and D-dimer were found in both groups. No significant changes in other fibrinolytic parameters or von Willebrand factor were found. No complications in terms of arterial or venous thrombosis were observed. Our pilot study suggests that long term, low-dose TXA treatment of haemodialysis patients with substantially prolonged in vitro closure time results in a significant improvement of platelet dysfunction and a significant increase in haemoglobin values. These new, promising results merit further investigation in larger studies.
- 1 Livio M, Marchesi D, Remuzzi G. Coagulation abnormalities in uraemia. Semin Nephrol 1985; 5: 82-90.
- 2 Eberst ME, Berkowitz LR. Haemostasis in renal disease: Pathophysiology and management. Am J Med 1994; 96: 168-79.
- 3 Rabelink TJ, Zwaginga JJ, Koomans HA. et al Thrombosis and haemostasis in renal disease. Kidney Int 1994; 46: 287-96.
- 4 Mezzano D, Tagle R, Panes O. et al Hemostatic disorder of uraemia: the platelet defect, main determinant of prolonged bleeding time, is correlated with indices of activation of coagulation and fibrinolysis. Thromb Haemost 1996; 76: 312-21.
- 5 Remuzzi G. Bleeding in renal failure. Lancet 1988; 1: 1205-8.
- 6 Weigert AL, Schafer AI. Uremic bleeding: pathogenesis and therapy. Am J Med Sci 1998; 316: 94-104.
- 7 Noris M, Remuzzi G. Uremic bleeding: closing the circle after 30 years of controversies?. Blood 1999; 94: 2569-74.
- 8 Zupan IP, Sabovic M, Salobir B. et al Utility of in vitro closure time test for evaluating platelet-related primary haemostasis in dialysis patients. Am J Kidney Dis 2003; 42: 746-51.
- 9 Favaloro EJ. Utility of the PFA-100 for assessing bleeding disorders and monitoring therapy: a review of analytical variables, benefits and limitations. Haemophilia 2001; 7: 170-9.
- 10 Kratzer MAA, Born GVR. Platelet function defects: simulation of primary haemostasis in vitro . Haemostasis 1985; 18: 167-85.
- 11 Kundu SK, Heilmann EJ, Sio R. et al Description of an in vitro platelet function analyzer PFA-100. Semin Thromb Haemost 1995; 21 (Suppl. 02) 106-12.
- 12 Mammen EF, Comp PC, Gosselin R. et al PFA-100TM System: a new method for assessment of platelet dysfunction. Semin Thromb Hemost 1998; 24: 195-202.
- 13 Marchant KK, Corcoran G. The laboratory diagnosis of platelet disorders. An algorithmic approach. Arch Pathol Lab Med 2002; 126: 133-46.
- 14 Nenci GG, Berrettini M, Agnelli G. et al The effect of peritoneal dialysis, hemodialysis and kidney transplantation on blood platelet function. I Platelet aggregation by ADP and epinephrine. Nephron 1979; 23: 287-92.
- 15 Remuzzi G, Livio M, Marchiaro G. et al Bleeding in renal failure: altered platelet function in chronic uraemia only partially corrected by haemodialysis. Nephron 1978; 22: 347-53.
- 16 George JN, Shatill SJ. The clinical importance of acquired abnormalities of platelet function. N Eng J Med 1991; 324: 27-39.
- 17 Kozek-Langenecker SA, Masaki T, Mohammad H. et al Fibrinogen fragments and platelet dysfunction in uraemia. Kidney Int 1999; 56: 299-305.
- 18 Mannucci PM. Hemostatis drugs. N Engl J Med 1998; 339: 245-53.
- 19 Hoylaerts M, Lijnen HR, Collen D. Studies on the mechanism of the antifibrinolytic action of tranexamic acid. Biochim Biophys Acta 1981; 673: 75-85.
- 20 Markus G, Priore RL, Wissler FC. The binding of tranexamic acid to native (Glu) and modified (Lys) human plasminogen and its effect on conformation. J Biol Chem 1979; 254: 1211-6.
- 21 Cyklokapron (Pharmacia). In: Krogh CME. (ed) CPS Compendium of pharmaceuticals and specialties. 28th ed.. Ottawa: Canadian Pharmaceutical Association; 1993: 311-2.
- 22 Mezzano D, Panes O, Munoz B. et al Tranexamic acid inhibits fibrinolysis, shortens the bleeding time and improves platelet function in patients with chronic renal failure. Thromb Haemost 1999; 82: 1250-4.
- 23 Wellington K, Wagstaff AJ. Tranexamic acid: a review of its use in the management of menorrhagia. Drugs 2003; 63: 1417-33.
- 24 Bonnar J, Sheppard BL. Treatment of menorrhagia during menstruation: randomised controlled trial of ethamsylate, mefenamic acid, and tranexamic acid. BMJ 1996; 313: 579-82.
- 25 Katsaros D, Petricevic M, Snow NJ. et al Tranexamic acid reduces postbypass blood use: a double blinded, prospective, randomized study of 210 patients. Ann Thorac Surg 1996; 1131-5.
- 26 Vujkovac B, Lavre J, Sabovic M. Successful treatment of bleeding from colonic angiodysplasias with tranexamic acid in a haemodialysis patient. Am J Kidney Disease 1998; 31: 536-8.
- 27 Vujkovac B, Sabovic M. Treatment of subdural and intracerebral hematomas in a haemodialysis patient with tranexamic acid. Nephrol Dialysis Transplant 2000; 15: 107-9.
- 28 Sabovic M, Lavre J, Vujkovac B. Tranexamic acid is beneficial as adjunctive therapy in treating major upper gastrointestinal bleeding in dialysis patients. Nephrol Dialysis Transplant 2003; 18: 1388-91.
- 29 Lindoff C, Rybo G, Astedt B. Treatment with tranexamic acid during pregnancies and the risk of thromboembolic complications. Thromb Haemost 1993; 70: 238-40.