Monitoring of fibrinolytic system activity with plasminogen, D-dimers and FDP in primary total knee arthroplasty (TKA) after topical, intravenous or combined administration of tranexamic acid.

Jiri Lostak,Jana Zapletalova,Ludek Slavik,Lubos Balaz,Jiri Gallo

doi:10.5507/bp.2019.034

Jiri Lostak, Jana Zapletalova + Show 3 more

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https://doi.org/10.5507/bp.2019.034

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Journal: Biomedical Papers	Publication Date: Sep 16, 2019
Citations: 7	License type: CC BY 4.0

Affiliation: Palacký University, Olomouc

Abstract

We assessed various ways of tranexamic acid (TXA) administration on the fibrinolytic system. Blood loss, transfusions, drainage and haematoma were secondary outcomes. In this prospective study, we examined 100 patients undergoing primary total knee arthroplasty (TKA) between June and November 2018. Patients were randomly assigned to 4 groups according to the following TXA regimens: 1) loading dose 15 mg TXA/kg single intravenous administration applied at initiation of anesthesia (IV1); 2) loading dose 15 mg TXA/kg + additional dose 15 mg TXA/kg 6 h after the first application of TXA (IV2); 3) IV1 regime in combination with a local wash of 2 g of TXA in 50 mL of saline (COMB); 4) topical administration of 2 g of TXA in 50 mL of saline (TOP). Systemic fibrinolysis interference was insignificant in all of the regimens; we did not detect significant differences between IV1, IV2 and COMB in the monitored parameters within the elapsed time after the TKA; IV regimes had the lowest total drainage blood loss; the lowest blood loss was associated with the IV1 and IV2 regimens (IV1, IV2 < COMB < TOP); the lowest incidence of haematomas was in patients treated with TXA topically (i.e., in COMB + TOP). The largest antifibrinolytic effect was associated with intravenous administration of TXA. In terms of blood loss, intravenously administered TXA can interfere with the processes associated with the formation of the fibrin plug more efficiently than the simple washing of wound surfaces with TXA.

Highlights

Tranexamic acid (TXA) is a synthetic amino acid derivative of lysine that inhibits the conversion of plasminogen to plasmin by blocking the binding site of plasminogen to a fibrin molecule
The pre-operative values of plasminogen, D-dimers and fibrinfibrinogen degradation products (FDP) corresponded to variability within the physiological standard
In the first 6 hours after the start of surgery, we observed significantly lower levels of fibrin cleavage products (D-dimers, FDP) in protocols where TXA was administered intravenously or in combination with topical administration (IV1, IV2, COMB) versus topical TXA, which had the least effect on systemic inhibition of fibri

Summary

Introduction

Tranexamic acid (TXA) is a synthetic amino acid derivative of lysine that inhibits the conversion of plasminogen to plasmin by blocking the binding site of plasminogen to a fibrin molecule. TXA can directly inhibit plasmin activity[1,2]. It is believed that TXA has an anti-inflammatory effect (inhibition of plasmin-mediated complement, monocyte and neutrophil inhibition)[3]. The effect of TXA is more potentiated by factor X (ref.[4]). TXA has gradually become a routine part of perioperative care in primary total arthroplasty of the hips and knees[5, 6]. Most studies were performed with systemic administration of TXA (ref.[1])

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