| Literature DB >> 26448897 |
Sophia Binz1, Jonathon McCollester2, Scott Thomas3, Joseph Miller1, Timothy Pohlman4, Dan Waxman5, Faisal Shariff6, Rebecca Tracy3, Mark Walsh7.
Abstract
This paper reviews the application of tranexamic acid, an antifibrinolytic, to trauma. CRASH-2, a large randomized controlled trial, was the first to show a reduction in mortality and recommend tranexamic acid use in bleeding trauma patients. However, this paper was not without controversy. Its patient recruitment, methodology, and conductance in moderate-to-low income countries cast doubt on its ability to be applied to trauma protocols in countries with mature trauma networks. In addition to traditional vetting in scientific, peer-reviewed journals, CRASH-2 came about at a time when advances in communication technology allowed debate and influence to be leveraged in new forms, specifically through the use of multimedia campaigns, social media, and Internet blogs. This paper presents a comprehensive view of tranexamic acid utilization in trauma from peer-reviewed evidence to novel multimedia influences.Entities:
Year: 2015 PMID: 26448897 PMCID: PMC4576020 DOI: 10.1155/2015/874920
Source DB: PubMed Journal: J Blood Transfus ISSN: 2090-9195
Randomized controlled trials involving TXA use.
| Study | Author(s) | Description | Year | Outcomes | Recommendations |
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| CRASH-2 [ | Shakur et al. | 20,211 pts with recruitment by “uncertainty principle” | 2010 | All-cause mortality 14.5% tranexamic acid (TXA) group versus 16.0% placebo group, | Tranexamic acid should be used in bleeding trauma patients |
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| PATCH [ | Gruen et al. | 1184 pts in shock determined by COAST criteria | July 2014 start date | Ongoing study | |
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| STAAMP [ | Universities of Pittsburgh, Rochester, Texas at San Antonio, and Utah | 1000 pts with prehospital shock and nonshock | July 2015 start date | Ongoing study | |
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| TAMPITI [ | Spinella and Bochicchio | 150 pts who received one blood product and/or immediate transfer to OR | Fall 2015–Spring 2017 | Ongoing study | |
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| Tranexamic Acid in Orthopaedic Trauma Surgery [ | Kiner | 100 pts with orthopaedic trauma (hip or knee) | May 2012–Dec. 2015 | Ongoing study | |
Review articles on TXA use in trauma.
| Title | Author(s) | Description | Year | Critique |
|---|---|---|---|---|
| Tranexamic Acid for Trauma Patients: A Critical Review of the Literature [ | Cap et al. | Systematic review of TXA | 2011 | Favorable towards CRASH-2 findings and recommends use in combat situations and bleeding trauma patients |
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| Tranexamic Acid and Trauma: Current Status and Knowledge Gaps with Recommended Research Priorities [ | Pusateri et al., Department of Defense | Systematic review of TXA | 2013 | Identifies “knowledge gaps” in the CRASH-2 trial: (1) lack of clarity of reporting of monitoring, complications, (2) no transfusion benefit, and (3) data not robust |
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| Tranexamic Acid in Trauma: How Should We Use It? [ | Napolitano et al. | Systematic review of TXA | 2013 | Major knowledge gaps: (1) recruitment, (2) 100% follow-up, (3) 50% received transfusion, (4) survival benefit not a function of transfusion, (5) TBI greatest cause of death, (6) low rate of thrombosis, and (7) other shortcomings noted |
Nonrandomized controlled trials on TXA use in trauma.
| Title | Author(s) | Description | Year | Outcomes | Recommendations |
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| Military Application of Tranexamic Acid in Trauma Emergency Resuscitation (MATTERs) study [ | Morrison et al. | Retrospective observational study; 896 pts with combat injury and at least one unit of PRBCs | 2011 | TXA significant survivor benefit with reduced blood utilization and increased rate of VTE | TXA should be incorporated into trauma resuscitation protocols for “severe wartime injury and hemorrhage” |
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| Tranexamic Acid Use in Trauma: Effective but Not without Consequences [ | Swendsen et al. | Retrospective multi cohort study; 126 trauma pts, 93 straight to OR/IR of whom 46 received TXA | 2013 | TXA mortality benefit, increased VTE, trend towards increased AKI, and no transfusions differences | “In civilian trauma, early TXA administration confers early survival advantage without affecting blood product usage but may increase the risk of DVT/PE and AKI” |
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| Do All Trauma Patients Benefit from Tranexamic Acid? [ | Valle et al. | Retrospective, observational single-center study; 1,217 trauma patients requiring OR/transfusions | 2014 | TXA group that had increased mortality, PRBCs, and crystalloid | “Prospective studies are needed to further identify conditions that may override the benefits from TXA” |
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| Tranexamic Acid Use in Severely Injured Civilian Patients and the Effects on Outcomes [ | Cole et al. | Prospective cohort study; 385 severely injured (ISS > 15), civilian pts. Focused on 131 shocked pts | 2015 | TXA mortality benefit for shocked patients not statistically significant; increased rate of VTE in TXA | TXA is recommended for “severely injured shocked patients” |
Editorials on TXA use.
| Title | Author | Description | Year | Outcomes | Recommendations |
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| CRASH-2 Goes Viral [ | The Lancet | Editorial (Internet) | 2011 | Reviews CRASH-2 media coverage | Recommends TXA in trauma |
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| Antifibrinolytics in trauma patients [ | Kenji Inaba | Editorial (Internet/print) | 2012 | Reviews | Cites CRASH-2 “challenges” and notes MATTERs clarity |
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| Trauma and Tranexamic Acid [ | Gruen et al. | Editorial (Print) | 2013 | Reviews knowledge gaps noted by | Recommends that TXA be confirmed in future RCTs |
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| CRASH2, MATTERS…TXA in Trauma [ | Mark Putland | Editorial (Internet/ blog) | 2013 | Reviews CRASH-2 MATTERs, MATTERs II | Data for seizures and thromboembolic complications remain incomplete. Needs more study. |