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(Completed journal club article: added exclusion criteria, baseline characteristics, full outcome data with RR/CI, subgroup analysis, expanded criticisms, references) |
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{{JC info | {{JC info | ||
| title=Effects of tranexamic acid on death, disability, vascular occlusive events and other morbidities in patients with acute traumatic brain injury (CRASH-3): a randomised, placebo-controlled trial | | title=Effects of tranexamic acid on death, disability, vascular occlusive events and other morbidities in patients with acute traumatic brain injury (CRASH-3): a randomised, placebo-controlled trial | ||
| abbreviation=CRASH-3 | | abbreviation=CRASH-3 | ||
| published=2019 | | expansion=Clinical Randomisation of an Antifibrinolytic in Significant Head injury 3 | ||
| author=The | | published=2019-10 | ||
| author=The CRASH-3 Trial Collaborators | |||
| journal=The Lancet | | journal=The Lancet | ||
| year=2019 | | year=2019 | ||
| volume | | volume=394 | ||
| | | issue=10210 | ||
| pages | | pages=1713-1723 | ||
| pmid= 31623894 | | pmid=31623894 | ||
| fulltexturl= | | fulltexturl=https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(19)32233-0/fulltext | ||
| status = | | pdfurl= | ||
| status = Complete | |||
}} | }} | ||
==Clinical Question== | ==Clinical Question== | ||
Does tranexamic acid reduce head injury-related death in patients with traumatic brain injury (TBI)? | |||
==Conclusion== | ==Conclusion== | ||
Tranexamic acid is safe in patients with TBI and, when administered within 3 hours of injury, reduces head injury-related death. The benefit is most apparent in patients with mild-to-moderate TBI (GCS 9-15) rather than those with severe TBI (GCS 3). Patients should be treated as soon as possible after injury. | |||
[[ | ==Major Points== | ||
*CRASH-3 was designed as a follow-up to the landmark [[EBQ:CRASH-2 Trial|CRASH-2 trial]] which demonstrated survival benefit of TXA in trauma patients with hemorrhage | |||
*The primary analysis showed a non-significant trend toward reduced head injury-related death with TXA (18.5% vs 19.8%; RR 0.94, 95% CI 0.86-1.02) | |||
*A prespecified sensitivity analysis excluding patients with GCS 3 or bilateral unreactive pupils (who had minimal potential to benefit) showed a more notable reduction (12.5% vs 14.0%; RR 0.89, 95% CI 0.80-1.00) | |||
*The effect was greatest in patients with '''mild-to-moderate TBI''' (GCS 9-15) | |||
*No increase in vascular occlusive events (MI, stroke, DVT, PE) was observed with TXA | |||
*The trial enrolled 12,737 patients across 175 hospitals in 29 countries, making it the largest TXA trial in TBI | |||
==Design== | ==Study Design== | ||
* | *Multicenter, randomized, double-blind, placebo-controlled trial | ||
*175 hospitals in 29 countries | |||
*12,737 patients randomized | |||
**TXA group: n=6,406 | |||
**Placebo group: n=6,331 | |||
*Intention-to-treat analysis | |||
*28-day follow-up | |||
==Population | ==Population== | ||
===Inclusion Criteria=== | ===Inclusion Criteria=== | ||
*Adults with TBI | *Adults with TBI | ||
*Within '''3 hours''' of injury | |||
*GCS '''12 or lower''' OR any intracranial bleeding on CT scan | |||
*No significant extracranial bleeding | |||
===Exclusion Criteria=== | ===Exclusion Criteria=== | ||
*Clear indication or contraindication to tranexamic acid | |||
*Significant extracranial hemorrhage | |||
===Baseline Characteristics=== | ===Baseline Characteristics=== | ||
*80% | *Male: ~80% | ||
*Mean age 41.7 years | *Mean age: 41.7 years | ||
*Bilateral nonreactive pupils 9% | *GCS 3-8: ~30% | ||
*GCS 9-12: ~20% | |||
*GCS 13-15 with intracranial bleeding: ~50% | |||
*Bilateral nonreactive pupils: ~9% | |||
*Intracranial bleeding on CT: ~75% | |||
== | ==Interventions== | ||
*'''TXA group''': Loading dose of 1g IV over 10 minutes, followed by 1g IV infusion over 8 hours | |||
*'''Placebo group''': Matching placebo (0.9% saline) | |||
* | |||
Prespecified sensitivity analysis | ==Outcomes== | ||
* | ===Primary Outcome=== | ||
*Head injury-related death in hospital within 28 days of injury: | |||
**TXA: 855/4613 (18.5%) | |||
**Placebo: 892/4514 (19.8%) | |||
**RR 0.94 (95% CI 0.86-1.02), p=0.14 | |||
*'''Prespecified sensitivity analysis''' (excluding GCS 3 and bilateral unreactive pupils): | |||
**TXA: 485/3880 (12.5%) | |||
**Placebo: 525/3757 (14.0%) | |||
**RR 0.89 (95% CI 0.80-1.00), p=0.047 | |||
===Secondary Outcomes=== | ===Secondary Outcomes=== | ||
*Early head injury-related death (within 24 | *All-cause mortality: No significant difference | ||
* | *Early head injury-related death (within 24 hours): Reduced with TXA (risk reduction most evident in this early period) | ||
*Disability (Disability Rating Scale): No significant difference | |||
*Vascular occlusive events (MI, CVA, DVT, PE) | *Vascular occlusive events (MI, CVA, DVT, PE): Similar in TXA vs placebo groups | ||
*Seizures | *Seizures: Similar between groups | ||
* | *Neurosurgical intervention: Similar between groups | ||
===Subgroup Analysis=== | |||
*Greatest benefit in patients with '''mild-to-moderate TBI''' (GCS 9-15) | |||
*Patients with severe TBI (GCS 3) and bilateral unreactive pupils showed minimal benefit | |||
*Benefit diminished with increasing time to treatment | |||
==Criticisms== | |||
== | *Primary outcome did not reach statistical significance in the full intention-to-treat analysis (p=0.14) | ||
*The prespecified sensitivity analysis (excluding GCS 3 and bilateral unreactive pupils) is what demonstrated significance, which weakens the overall conclusion | |||
*Potential for undersensing adverse events (thrombotic events) since a diagnostic test was required to confirm the event | |||
*The trial was designed for a larger treatment effect than was observed, suggesting it may have been underpowered for the primary outcome | |||
*Majority of patients had mild-to-moderate TBI; applicability to severe TBI remains uncertain | |||
*Different from CRASH-2 in that TBI patients have different pathophysiology of coagulopathy compared to hemorrhagic shock | |||
==Funding== | ==Funding== | ||
National | *National Institute for Health Research Health Technology Assessment | ||
*JP Moulton Charitable Trust | |||
*Department of Health and Social Care | |||
*Department for International Development | |||
*Global Challenges Research Fund | |||
*Medical Research Council | |||
*Wellcome Trust (Joint Global Health Trials Scheme) | |||
==See Also== | ==See Also== | ||
*[[EBQ:CRASH-2 Trial]] | |||
*[[Traumatic brain injury]] | |||
*[[Intracranial hemorrhage]] | |||
==References== | |||
*CRASH-3 trial collaborators. Effects of tranexamic acid on death, disability, vascular occlusive events and other morbidities in patients with acute traumatic brain injury (CRASH-3): a randomised, placebo-controlled trial. ''Lancet''. 2019;394(10210):1713-1723. PMID 31623894 | |||
Revisión actual - 22:09 21 mar 2026
Complete Journal Club Article
The CRASH-3 Trial Collaborators. "Effects of tranexamic acid on death, disability, vascular occlusive events and other morbidities in patients with acute traumatic brain injury (CRASH-3): a randomised, placebo-controlled trial". The Lancet. 2019. 394(10210):1713-1723.
PubMed Full text
PubMed Full text
Clinical Question
Does tranexamic acid reduce head injury-related death in patients with traumatic brain injury (TBI)?
Conclusion
Tranexamic acid is safe in patients with TBI and, when administered within 3 hours of injury, reduces head injury-related death. The benefit is most apparent in patients with mild-to-moderate TBI (GCS 9-15) rather than those with severe TBI (GCS 3). Patients should be treated as soon as possible after injury.
Major Points
- CRASH-3 was designed as a follow-up to the landmark CRASH-2 trial which demonstrated survival benefit of TXA in trauma patients with hemorrhage
- The primary analysis showed a non-significant trend toward reduced head injury-related death with TXA (18.5% vs 19.8%; RR 0.94, 95% CI 0.86-1.02)
- A prespecified sensitivity analysis excluding patients with GCS 3 or bilateral unreactive pupils (who had minimal potential to benefit) showed a more notable reduction (12.5% vs 14.0%; RR 0.89, 95% CI 0.80-1.00)
- The effect was greatest in patients with mild-to-moderate TBI (GCS 9-15)
- No increase in vascular occlusive events (MI, stroke, DVT, PE) was observed with TXA
- The trial enrolled 12,737 patients across 175 hospitals in 29 countries, making it the largest TXA trial in TBI
Study Design
- Multicenter, randomized, double-blind, placebo-controlled trial
- 175 hospitals in 29 countries
- 12,737 patients randomized
- TXA group: n=6,406
- Placebo group: n=6,331
- Intention-to-treat analysis
- 28-day follow-up
Population
Inclusion Criteria
- Adults with TBI
- Within 3 hours of injury
- GCS 12 or lower OR any intracranial bleeding on CT scan
- No significant extracranial bleeding
Exclusion Criteria
- Clear indication or contraindication to tranexamic acid
- Significant extracranial hemorrhage
Baseline Characteristics
- Male: ~80%
- Mean age: 41.7 years
- GCS 3-8: ~30%
- GCS 9-12: ~20%
- GCS 13-15 with intracranial bleeding: ~50%
- Bilateral nonreactive pupils: ~9%
- Intracranial bleeding on CT: ~75%
Interventions
- TXA group: Loading dose of 1g IV over 10 minutes, followed by 1g IV infusion over 8 hours
- Placebo group: Matching placebo (0.9% saline)
Outcomes
Primary Outcome
- Head injury-related death in hospital within 28 days of injury:
- TXA: 855/4613 (18.5%)
- Placebo: 892/4514 (19.8%)
- RR 0.94 (95% CI 0.86-1.02), p=0.14
- Prespecified sensitivity analysis (excluding GCS 3 and bilateral unreactive pupils):
- TXA: 485/3880 (12.5%)
- Placebo: 525/3757 (14.0%)
- RR 0.89 (95% CI 0.80-1.00), p=0.047
Secondary Outcomes
- All-cause mortality: No significant difference
- Early head injury-related death (within 24 hours): Reduced with TXA (risk reduction most evident in this early period)
- Disability (Disability Rating Scale): No significant difference
- Vascular occlusive events (MI, CVA, DVT, PE): Similar in TXA vs placebo groups
- Seizures: Similar between groups
- Neurosurgical intervention: Similar between groups
Subgroup Analysis
- Greatest benefit in patients with mild-to-moderate TBI (GCS 9-15)
- Patients with severe TBI (GCS 3) and bilateral unreactive pupils showed minimal benefit
- Benefit diminished with increasing time to treatment
Criticisms
- Primary outcome did not reach statistical significance in the full intention-to-treat analysis (p=0.14)
- The prespecified sensitivity analysis (excluding GCS 3 and bilateral unreactive pupils) is what demonstrated significance, which weakens the overall conclusion
- Potential for undersensing adverse events (thrombotic events) since a diagnostic test was required to confirm the event
- The trial was designed for a larger treatment effect than was observed, suggesting it may have been underpowered for the primary outcome
- Majority of patients had mild-to-moderate TBI; applicability to severe TBI remains uncertain
- Different from CRASH-2 in that TBI patients have different pathophysiology of coagulopathy compared to hemorrhagic shock
Funding
- National Institute for Health Research Health Technology Assessment
- JP Moulton Charitable Trust
- Department of Health and Social Care
- Department for International Development
- Global Challenges Research Fund
- Medical Research Council
- Wellcome Trust (Joint Global Health Trials Scheme)
See Also
References
- CRASH-3 trial collaborators. Effects of tranexamic acid on death, disability, vascular occlusive events and other morbidities in patients with acute traumatic brain injury (CRASH-3): a randomised, placebo-controlled trial. Lancet. 2019;394(10210):1713-1723. PMID 31623894