EBQ:Halt It Trial

incomplete Journal Club Article

Roberts I, Shakur-Still H, Afolabi A, et al.. "Effects of a high-dose 24-h infusion of tranexamic acid on death and thromboembolic events in patients with acute gastrointestinal bleeding (HALT-IT): an international randomised, double-blind, placebo-controlled trial". Lancet. 2020. 395(10241):1927-1936.
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Clinical Question

Does high-dose IV tranexamic acid reduce death due to bleeding within five days in adult patients with acute gastrointestinal bleeding compared to placebo?

Conclusion

Tranexamic acid confers no benefit on 5-day mortality due to bleeding in adult patients with acute GI bleed.

Major Points

Tranexamic acid (TXA) is a synthetic lysine derivative that decreases fibrinolysis by inhibiting the conversion of plasminogen to plasmin. It has been used broadly in trauma patients with hemodynamically significant bleeding and appears to confer a mortality benefit in this population^[1]. A prior systematic review of TXA for use in acute gastrointestinal bleeding suggested a mortality benefit, although the review was based on a series of small studies prone to bias^[2].

HALT-IT is the first large, pragmatic, international, double-blind RCT to systematically evaluate the use of TXA in acute undifferentiated GI bleed. In this study, patients that received TXA 1g IV loading dose followed by a 3g infusion over 24 hours had the same mortality rate from bleeding at five days as patients receiving a matching normal saline placebo (222 [3.7%] intervention group vs 226 [3.8%] placebo, RR 0.99). All-cause mortality at 28 days was also no different between groups. There was a suggestion of increased venous thromboembolic events in the TXA group (48 [0.8%] vs 26 [0.4%], RR 1.85 [CI 1.15-2.98]).

Study Design

Large, pragmatic, multicenter international placebo-controlled RCT, conducted at 164 hospitals in 15 countries

12,009 patients enrolled with acute GI bleeding
- Tranexamic acid (n=5,994)
  - Placebo (n=6,015)

Population

Patient Demographics

Patients older (mean age 58), male (65%), and mostly upper GI bleeds (90%)
Mean time to randomization from onset of bleeding 22h
Most patients (57%) did not display signs of shock on initial presentation

Inclusion Criteria

Adult patients with acute gastrointestinal bleeding
Clinician defined bleeding as significant, meaning possibility of death from bleeding
- Age of inclusion either 16 or 18 depending on definition of "adult" in home country
Clinician had to be "uncertain" whether or not to use TXA

Exclusion Criteria

Clinician-determined clear indication for TXA
Clinician-determined clear contraindication for TXA

Interventions

TXA 1g IV over 10 minloading dose followed by a 3g infusion in NS over 24 hours

Outcomes

Primary Outcome

Death from bleeding at 5 days
- No difference between TXA (222, 3.7%)and placebo (226, 3.8%)

Secondary Outcomes

All-cause mortality at 28 days
- Originally was the primary outcome, replaced by the above (see discussion)
- No difference between TXA (9.5%) and placebo (9.2%), RR 1·03, 95% CI 0·92– 1.16
No difference in rebleeding, need for endoscopy/surgery, transfusion requirement, or mortality from other subgroups (i.e. infection, organ failure, etc)
Thromboembolic events
- Any: 1.4% in TXA group vs 1.2% in placebo (RR 1.20, 95% CI 0.88-1.64)
- Venous (DVT and PE): 0.8% in TXA group vs 0.4% in placebo (RR 1.85, 95% CI 1.15-2.98)
Seizures
- 0.6% in TXA group vs 0.4% in placebo (RR 1.73, 95% CI 1.03-2.93

Subgroup analysis

4 preplanned subgroups within the primary outcome:

Time from onset of bleeding, greater or less than 3h
Site of bleed, upper or lower
Varices and comorbid liver disease vs other causes of bleeding
Rockall score

TXA showed no benefit in any subgroup.

Criticisms & Further Discussion

Previous positive studies of TXA on GI bleeds have been small or observational and subject to bias
This large RCT is well-designed, pragmatic, and answers a clinically relevant question
The study authors changed the original primary outcome from all-cause 28-day mortality to death due to bleeding at 5 days
- During an interim analysis authors noted that >50% of deaths were from non-hemorrhagic causes
- New primary outcome is disease-specific and at the judgment of the clinician
Patients for whom TXA was thought to be "clearly indicated" were excluded from the trial
- Some sicker patients who could have benefited from TXA may have been excluded
Time to randomization was long (22 hours on average); CRASH-2 signaled that earlier administration of TXA is better
- However, GI bleed patients tend to present roughly in the timeframe represented in the trial

External Links

Funding

The UK National Institute for Health Research Health Technology Assessment Programme

References

↑ Roberts I et al. Effects of a high-dose 24-h infusion of tranexamic acid on death and thromboembolic events in patients with acute gastrointestinal bleeding (HALT-IT): an international randomised, double-blind, placebo-controlled trial. The Lancet. 2020; 395(10241):1927-1936
↑ Bennett C, Klingenberg SL, Langholz E, Gluud LL. Tranexamic acid for upper gastrointestinal bleeding. The Cochrane database of systematic reviews. 2014

Authors:

[1] Roberts I et al. Effects of a high-dose 24-h infusion of tranexamic acid on death and thromboembolic events in patients with acute gastrointestinal bleeding (HALT-IT): an international randomised, double-blind, placebo-controlled trial. The Lancet. 2020; 395(10241):1927-1936

[2] Bennett C, Klingenberg SL, Langholz E, Gluud LL. Tranexamic acid for upper gastrointestinal bleeding. The Cochrane database of systematic reviews. 2014

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