Effect of the administration route on the hemostatic efficacy of tranexamic acid in patients undergoing short-segment posterior lumbar interbody fusion: a systematic review and meta-analysis

Matthew J Hatter; Zach Pennington; Timothy I Hsu; Tara Shooshani; Olivia Yale; Omead Pooladzandi; Sean S Solomon; Bryce Picton; Marlena Ramanis; Nolan J Brown; Sohaib Hashmi; Yu-Po Lee; Nitin Bhatia; Martin H Pham

doi:10.3171/2024.2.SPINE23779

Effect of the administration route on the hemostatic efficacy of tranexamic acid in patients undergoing short-segment posterior lumbar interbody fusion: a systematic review and meta-analysis

J Neurosurg Spine. 2024 May 17:1-12. doi: 10.3171/2024.2.SPINE23779. Online ahead of print.

Authors

Matthew J Hatter^{1

2}, Zach Pennington³, Timothy I Hsu², Tara Shooshani², Olivia Yale², Omead Pooladzandi⁴, Sean S Solomon^{1

2}, Bryce Picton^{2

5}, Marlena Ramanis^{1

2}, Nolan J Brown⁵, Sohaib Hashmi¹, Yu-Po Lee¹, Nitin Bhatia¹, Martin H Pham⁶

Affiliations

¹ Departments of1Orthopedic Surgery and.
² 2University of California Irvine School of Medicine, Irvine, California.
³ 3Department of Neurologic Surgery, Mayo Clinic, Rochester, Minnesota.
⁴ 5Department of Electrical and Computer Engineering, University of California, Los Angeles, California; and.
⁵ 4Neurosurgery, University of California Irvine, Orange, California.
⁶ 6Department of Neurosurgery, University of California-San Diego School of Medicine, La Jolla, California.

PMID: 38759242
DOI: 10.3171/2024.2.SPINE23779

Abstract

Objective: Tranexamic acid (TXA) is an FDA-approved antifibrinolytic that is seeing increased popularity in spine surgery owing to its ability to reduce intraoperative blood loss (IOBL) and allogeneic transfusion requirements. The present study aimed to summarize the current literature on these formulations in the context of short-segment instrumented lumbar fusion including ≥ 1-level posterior lumbar interbody fusion (PLIF).

Methods: The PubMed, Cochrane, and Web of Science databases were queried for all full-text English studies evaluating the use of topical TXA (tTXA), systemic TXA (sTXA), or combined tTXA+sTXA in patients undergoing PLIF. The primary endpoints of interest were operative time, IOBL, and total blood loss (TBL); secondary endpoints included venous thromboembolic complication occurrence, and allogeneic and autologous transfusion requirements. Outcomes were compared using random effects. Comparisons were made between the following treatment groups: sTXA, tTXA, and sTXA+tTXA. Given that sTXA is arguably the standard of care in the literature (i.e., the most common route of administration that to this point has been studied the most), the authors compared sTXA versus tTXA and sTXA versus sTXA+tTXA. Study heterogeneity was assessed with the I2 test, and grouped analysis using the Hedge's g test was performed for measurement of effect size.

Results: Forty-five articles were identified, of which 17 met the criteria for inclusion with an aggregate of 1008 patients. TXA regimens included sTXA only, tTXA only, and various combinations of sTXA and tTXA. There were no significant differences in operative time, TBL, or postoperative drainage between the sTXA and tTXA groups or between the sTXA and sTXA+tTXA groups.

Conclusions: The present meta-analysis suggested clinical equipoise between isolated sTXA, isolated tTXA, and combinatorial tTXA+sTXA formulations as hemostatic adjuvants/neoadjuvants in short-segment fusion including ≥ 1-level PLIF. Given the theoretically lower venous thromboembolism risk associated with tTXA, additional investigations using large cohorts comparing these two formulations within the posterior fusion population are merited. Although TXA has been shown to be effective, there are insufficient data to support topical or systemic administration as superior within the open PLIF population.

Keywords: DVT; PLIF; antifibrinolytic; deep vein thrombosis; degenerative; estimated blood loss; hidden blood loss; intravenous; perioperative blood loss; posterior lumbar interbody fusion; route of administration; topical; tranexamic acid.