Effect of Out-of-Hospital Tranexamic Acid vs Placebo on 6-Month Functional Neurologic Outcomes in Patients With Moderate or Severe Traumatic Brain Injury

Effect of Out-of-Hospital Tranexamic Acid vs Placebo on 6-Month Functional Neurologic Outcomes in Patients With Moderate or Severe Traumatic Brain Injury

Dec 01, 2020
Katherine Wagner, MD and Jamie Sue Ullman, MD, Manhasset, NY
Cerebrovascular Neurosurgery Watch - Retired February 2023 Neurosurgery Watch

Background: Fibrinolysis peaks 3 hours after traumatic brain injury (TBI). Tranexamic acid (TXA), an anti-fibrinolytic agent, may mitigate this and prevent subsequent hematoma expansion.

Randomized, multicenter clinical trial enrolling 966 patients at 20 trauma centers in the US and Canada, from May 2015 - November 2017.

Patients were randomized to three groups:

Out-of-hospital TXA bolus (1 gram) and in-hospital bolus (1 gram) over 8 hours (bolus maintenance group, n=312)

Out-of-hospital TXA bolus (2 grams) and in-hospital placebo infusion over 8 hours (bolus only group, n=345)

Out of hospital placebo bolus and in-hospital placebo bolus (placebo group, n=309)

Treatment started within two hours of injury

The two-gram bolus dosing was trialed to evaluate its potential usefulness in prehospital and military settings, while the one-gram bolus dosing was based on the CRASH-2 trial.

Primary outcome was favorable neurologic function at 6 months (Glascow Outcome Scale- Extended > 4, corresponding to either moderate disability or good recovery).

Ultimately, the two TXA groups were combined and compared to the placebo group to ensure adequate power.

1063 patients randomized, 966 participated (96 did not receive the study drug, one was excluded later).

Mean age 43 years old, 74% male, mean Glascow Coma Scale 8

The all-cause 28-day mortality was 14% in the combined TXA groups and 17% in the placebo group; this result was not statistically significant (p=0.26).

This result differs from what the CRASH-3 authors found for patients with mild to moderate TBI (see link in Sources).

The difference in the primary outcome of favorable neurologic outcome between the TXA groups and placebo group was -3.5%, (65% vs 62%, p=0.16 for benefit). This result was not statistically significant.

There were more thrombotic events in the bolus only and placebo groups (9% and 10%, respectively) than in the bolus maintenance group (4%).

Bolus only patients were also more likely to experience seizures (5% versus 2% in the other two groups), but they received fewer blood transfusions than patients in the other groups.

Source
JAMA

doi: 10.1001/jama.2020.8958

The Lancet (CRASH-3)

doi.org/10.1016/S0140-6736(19)32312-8

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