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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02187120
Other study ID # APP1044894
Secondary ID U1111-1160-6738
Status Completed
Phase Phase 3
First received
Last updated
Start date July 28, 2014
Est. completion date September 7, 2022

Study information

Verified date January 2023
Source Monash University
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this research is to determine whether giving severely injured adults a drug called tranexamic acid (TXA) as soon as possible after injury will improve their chances of survival and their level of recovery at six months. After severe injury, a person may have uncontrolled bleeding that places them at high risk of bleeding to death. Coagulation (the formation of blood clots) is an important process in the body that helps to control blood loss. Up to a quarter of people that are severely injured have a condition called acute traumatic coagulopathy. This condition affects coagulation and results in the break down of blood clots (fibrinolysis) that can lead to increased blood loss and an increased risk of dying. TXA is an anti-fibrinolytic drug that might help to reduce the effects of acute traumatic coagulopathy by preventing blood clots from breaking down and helping to control bleeding. In Australia, TXA is approved for use by the Therapeutic Goods Administration (TGA) to reduce blood loss or the need for blood transfusion in patients undergoing surgery (i.e. cardiac surgery, knee or hip arthroplasty). Recent evidence from a large clinical trial (CRASH-2) showed early treatment with TXA reduced the risk of death in severely injured patients, however the majority of patients involved in the study were injured in countries where prehospital care is limited and rapid access to lifesaving treatments is limited compared to that available in countries like Australia and New Zealand. It is unclear whether TXA will reduce the risk of death to the same degree when it is given alongside other lifesaving treatments that are available to patients soon after injury in these countries. The hypothesis is that TXA given early to injured patients who are at risk of acute traumatic coagulopathy and who are treated in countries with systems providing advanced trauma care reduces mortality and improves recovery at 6-months after injury.


Recruitment information / eligibility

Status Completed
Enrollment 1310
Est. completion date September 7, 2022
Est. primary completion date May 9, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Adult patients (estimated age 18 years or older) - Injured through any mechanism - Coagulopathy of severe trauma (COAST) score of 3 points or greater - First dose of study drug can be administered within three hours of injury - Patients to be transported to a participating trauma centre COAST score - Entrapment (ie in vehicle) [Yes = 1, No = 0] - Systolic blood pressure [<90 mmHg = 2, <100 mmHg = 1, =100 mmHg = 0] - Temperature [<32? =2, <35? = 1, =35? = 0] - Major chest injury likely to require intervention (e.g. decompression, chest tube) [Yes = 1, No = 0] - Likely intra-abdominal or pelvic injury [Yes = 1, No = 0] Exclusion Criteria: - Suspected pregnancy - Nursing home residents

Study Design


Intervention

Drug:
Tranexamic Acid
Tranexamic acid is a synthetic lysine derivative that inhibits fibrinolysis by blocking the lysine binding sites on plasminogen therefore inhibiting the conversion of plasminogen to plasmin. Intravenous injection of 1g Tranexamic Acid will be administered in the pre-hospital setting followed by 1g Tranexamic Acid infused intravenously over 8 hours initiated in the hospital emergency department.
Placebo


Locations

Country Name City State
Australia Royal Adelaide Hospital Adelaide South Australia
Australia Flinders Medical Centre Bedford Park South Australia
Australia Princess Alexandra Hospital Brisbane Queensland
Australia Royal Brisbane and Women's Hospital Brisbane Queensland
Australia Royal Darwin Hospital Darwin Northern Territory
Australia St John Ambulance Darwin Northern Territory
Australia South Australia Ambulance Service Eastwood South Australia
Australia St John Ambulance Western Australia Geraldton Western Australia
Australia Gold Coast Hospital Gold Coast Queensland
Australia Ambulance Tasmania Hobart Tasmania
Australia Royal Hobart Hospital Hobart Tasmania
Australia Queensland Ambulance Service Kedron Queensland
Australia Lismore Base Hospital Lismore New South Wales
Australia NNSW Medical Retrieval Service Lismore New South Wales
Australia Ambulance Victoria Melbourne Victoria
Australia Royal Melbourne Hospital Melbourne Victoria
Australia The Alfred Hospital Melbourne Victoria
Australia John Hunter Hospital Newcastle New South Wales
Australia CareFlight Northmead New South Wales
Australia Orange Base Hospital Orange New South Wales
Australia Royal Perth Hospital Perth Western Australia
Australia Ambulance Service of New South Wales Rozelle New South Wales
Australia Royal North Shore Hospital St Leonards New South Wales
Australia Liverpool Hospital Sydney New South Wales
Australia Wagga Wagga Base Hospital Wagga Wagga New South Wales
Australia Westmead Hospital Westmead New South Wales
New Zealand St John Ambulance Albany
New Zealand Auckland City Hospital Auckland
New Zealand Middlemore Hospital Auckland
New Zealand Waikato Hospital Hamilton West
New Zealand Hawke's Bay Hastings
New Zealand Wellington Free Ambulance Wellington
New Zealand Wellington Hospital Wellington

Sponsors (3)

Lead Sponsor Collaborator
Monash University Health Research Council, New Zealand, National Health and Medical Research Council, Australia

Countries where clinical trial is conducted

Australia,  New Zealand, 

References & Publications (5)

Gruen RL, Jacobs IG, Reade MC; PATCH-Trauma study. Trauma and tranexamic acid. Med J Aust. 2013 Sep 2;199(5):310-1. doi: 10.5694/mja13.10747. No abstract available. — View Citation

Gruen RL, Mitra B. Tranexamic acid for trauma. Lancet. 2011 Mar 26;377(9771):1052-4. doi: 10.1016/S0140-6736(11)60396-6. No abstract available. — View Citation

Mitra B, Cameron PA, Mori A, Maini A, Fitzgerald M, Paul E, Street A. Early prediction of acute traumatic coagulopathy. Resuscitation. 2011 Sep;82(9):1208-13. doi: 10.1016/j.resuscitation.2011.04.007. Epub 2011 Apr 21. — View Citation

Mitra B, Mazur S, Cameron PA, Bernard S, Burns B, Smith A, Rashford S, Fitzgerald M, Smith K, Gruen RL; PATCH-Trauma Study Investigators. Tranexamic acid for trauma: filling the 'GAP' in evidence. Emerg Med Australas. 2014 Apr;26(2):194-7. doi: 10.1111/1742-6723.12172. — View Citation

Reade MC, Pitt V, Gruen RL. Tranexamic acid and trauma: current status and knowledge gaps with recommended research priorities. Shock. 2013 Aug;40(2):160-1. doi: 10.1097/SHK.0b013e31829ab240. No abstract available. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Other Blood lactate concentration Immediately upon patient arrival to hospital
Other Laboratory analysis of fibrinolytic activity At the end of 8 hour infusion of study drug
Other Laboratory analysis of fibrinolytic activity 24 hours after first (prehospital) dose of study drug
Other Laboratory analysis of plasmin/anti-plasmin complexes At the end of 8 hour infusion of study drug
Other Laboratory analysis of plasmin/anti-plasmin complexes 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of tissue type plasminogen activator (tPA) At the end of 8 hour infusion of study drug
Other Laboratory analysis of tissue type plasminogen activator (tPA) 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of plasminogen activator inhibitor 1 (PAI-1) At the end of 8 hour infusion of study drug
Other Laboratory analysis of plasminogen activator inhibitor 1 (PAI-1) 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of t-PA/PAI-1 complexes Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of t-PA/PAI-1 complexes Substudy 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of thrombin activatable fibrinolysis inhibitor (TAFI) Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of thrombin activatable fibrinolysis inhibitor (TAFI) Substudy 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of interleukins (IL-2, IL-4, IL-6, IL-8, IL-10) Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of interleukins (IL-2, IL-4, IL-6, IL-8, IL-10) Substudy 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of granulocyte macrophage colony-stimulating factor (GM-CSF) Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of granulocyte macrophage colony-stimulating factor (GM-CSF) Substudy 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of interferon gamma Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of interferon gamma Substudy 24 hours after first (pre-hospital) dose of study drug
Other Laboratory analysis of tumour necrosis factor alpha Substudy At the end of 8 hour infusion of study drug
Other Laboratory analysis of tumour necrosis factor alpha Substudy 24 hours after first (pre-hospital) dose of study drug
Other TXA concentration in blood substudy 8 hours after first dose of study drug
Other TXA concentration in blood substudy 24 hours after first dose of study drug
Primary The proportion of patients with a favourable outcome (moderate disability or good recovery, GOSE scores 5-8) compared to those who have died (GOSE 1), or have severe disability (GOSE 2-4). 6 months
Secondary Units of blood products used (red blood cells, plasma, platelets, prothrombin complex concentrate, fibrinogen, Factor VIIa, cryoprecipitate) 24 hours
Secondary Coagulation assessed using the international normalised ratio (INR) Immediately upon patient arrival to hospital
Secondary Coagulation assessed using the international normalised ratio (INR) At the end of 8 hour infusion of study drug
Secondary Coagulation assessed using the international normalised ratio (INR) 24 hours after pre-hospital dose of study drug
Secondary Coagulation assessed by activated partial thromboplastin time (APTT) Immediately upon patient arrival to hospital
Secondary Coagulation assessed by activated partial thromboplastin time (APTT) At the end of 8 hour infusion of study drug
Secondary Coagulation assessed by activated partial thromboplastin time (APTT) 24 hours after pre-hospital dose of study drug
Secondary Platelet count Immediately upon patient arrival to hospital
Secondary Platelet count At the end of 8 hour infusion of study drug
Secondary Platelet count 24 hours after pre-hospital dose of study drug
Secondary Vascular occlusive events (myocardial infarction, stroke, deep venous thrombosis (DVT), pulmonary embolus (PE)) Hospital discharge (or up to 28 days in hospital)
Secondary Ventilator-free days 28 days
Secondary Mortality 24 hours
Secondary Mortality 28 days
Secondary Mortality 6 months
Secondary Proportion of deaths due to bleeding, vascular occlusion (pulmonary embolus, stroke, acute myocardial infarction), multi-organ failure, or head injury 24 hours
Secondary Proportion of deaths due to bleeding, vascular occlusion (pulmonary embolus, stroke, acute myocardial infarction), multi-organ failure, or head injury 28 days
Secondary Proportion of deaths due to bleeding, vascular occlusion (pulmonary embolus, stroke, acute myocardial infarction), multi-organ failure, or head injury 6 months
Secondary Cumulative incidence of sepsis Hospital discharge (or up to 28 days in hospital)
Secondary Quality of life measured using WHODAS 2.0 6 months
Secondary Quality of life measured using the EuroQOL 5 dimensions questionnaire (EQ-5D) 6 months
Secondary Number of participants with serious adverse events hospital discharge (or up to 28 days in hospital)
Secondary Coagulation assessed by fibrinogen Immediately upon patient arrival to hospital
Secondary Coagulation assessed by fibrinogen At the end of 8 hour infusion of study drug
Secondary Coagulation assessed by fibrinogen 24 hours after pre-hospital dose of study drug
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