Topical Tranexamic Acid in Major Paediatric Spine Deformity Surgery: A Randomized Controlled Trial

Blood loss during major paediatric spine surgery is significant, and it is well established that patients undergoing such surgery have a substantial risk for requiring a blood transfusion in the perioperative period (1-4). Given the cost and associated risks with allogeneic blood product transfusion (5-7), a significant effort has been directed towards reducing transfusion requirements through various methods of blood conservation (8-12).

Tranexamic acid (TXA) is a synthetic antifibrinolytic that functions through competitive blockade of the lysine-binding sites of plasminogen, plasmin, and tissue plasminogen activator resulting in the inhibition of fibrinolysis and clot degradation (13). When used parentally, it has been shown to safe, efficacious, and effective in reducing transfusion requirements and blood loss during the perioperative period of various orthopaedic procedures, including major surgeries of the spine (14-23). A growing body of literature has supported the topical application of TXA in lower extremity joint reconstruction, among other procedures (24-29), in which a saline solution containing TXA is placed directly in the surgical incision prior to closure. Two randomized controlled trials have compared topical TXA and placebo for use in lumbar fusion and laminectomy cases. Both of these trials demonstrated a significant reduction in perioperative blood loss with the use of topical TXA as compared to placebo, and no reported no adverse events (36, 37).

While intravenous TXA has proven efficacy in reducing perioperative blood loss, despite its routine use during major paediatric spine surgery, blood loss and transfusion requirements remain significant (14-23). Thus, methods to further reduce perioperative blood loss in the children are of clinical significance. As highlighted above, topical TXA has clearly demonstrated excellent local anti-fibrinolytic action. Furthermore, when applied within a surgical incision, there is a negligible increase in serum TXA concentration (33-35).

We therefore propose a randomized trial to evaluate the effect of topical TXA on perioperative blood loss when used in addition to intravenous TXA for major paediatric spine surgery. In doing so, we seek to evaluate whether additional benefit may be conferred through direct application of TXA within the incision intravenous to that already provided by IV TXA. To date, such a question has not been evaluated in the surgical literature.