BACKGROUND AND SCIENTIFIC RATIONALE. Protocol Code: ISRCTN V 1.0 date 30 Jan 2012

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BACKGROUND AND SCIENTIFIC RATIONALE Protocol Code: ISRCTN15088122 V 1.0 date 30 Jan 2012

Traumatic Brain Injury 10 million killed or hospitalised every year 90% in low and middle income countries Mostly young adults and long lasting disability The incidence of TBI is predicted to rise Bruns J, Hauser W. The epidemiology of traumatic brain injury: a review. Epilepsia 2003;44: Supplement 10:2 10. Peden M, Scurfield R, Sleet D, et al. World Report on Road Traffic Injury Prevention. Geneva: World Health Organization, 2004.

Rankings of Deaths & DALYs: 1990 2020 Deaths DALYs 1990 rank 2020 rank 1990 rank 2020 rank Road Traffic Injuries 9 6 9 3 Self Inflicted Injuries 12 10 17 14 Interpersonal Violence 16 14 19 12 War 20 15 16 8 If current trends continue, road traffic and intentional injuries will all rank in the 15 leading causes of death and burden of disease. Murray CJL, Lopez AD. Global health statistics: a compendium of incidence, prevalence and mortality estimates for over 200 conditions. Harvard School of Public Health, Boston: Harvard University Press, 1996. 3

Traumatic Brain Injury

Summary of relative risks for death at the end of studies on mannitol, hyperventilation, and barbiturates. Ker K et al. BMJ 2008;337:bmj.a865 2008 by British Medical Journal Publishing Group

Traumatic Brain Injury What works in head injury? We don t know Large treatment effects unlikely But even moderate effects worthwhile

Traumatic Brain Injury To detect moderate effects trials must be Large Well designed

A large simple placebo controlled trial, among adults with head injury and impaired consciousness, of the effects of a 48 hour infusion of corticosteroids on death and neurological disability

Death within 14 days Corticosteroidallocated Placeboallocated 1 052 / 4 985 (21.1%) 893 / 4 979 (17.9%) 1.18 (1.09 1.27) p < 0.001 0.8 1 1.2 1.4 1.6 Corticosteroid better Corticosteroid worse

9 October 2004

TXA and bleeding TXA reduces bleeding in surgery Transfusion Mortality RR (95% CI) RR (95% CI) TXA 0.62 (0.58-0.65) TXA 0.61 (0.38-0.98) 0.4 0.8 1.2 1.6 TXA better 95 trials TXA worse 0 0.4 0.8 1.2 1.6 TXA better TXA worse 72 trials Ker et al. BMC Emergency Medicine 2012, 12:3

CRASH 2 trial profile 20,211 randomised 10,096 allocated TXA 10,115 allocated placebo 3 consent withdrawn 1 consent withdrawn 10,093 baseline data 10,114 baseline data 33 lost to follow up Followed up = 10,060 (99.7%) 47 lost to follow up Followed up = 10,067 (99.5%)

Tranexamic acid and trauma TXA allocated (n=10,060) 1,463 (14.5%) Placebo allocated (n=10,067) 1,613 (16.0%) Risk ratio (95% CI) 0.91 (0.85 0.97) 2P=0.0035 0.8 0.9 1.0 1.1 TXA better TXA worse The CRASH 2 Collaborators. Effects of tranexamic acid on death, vascular occlusive events, and blood transfusion in trauma patients with significant haemorrhage (CRASH 2): a randomised, placebo controlled trial. The Lancet. 2010; 376(9734):23 32.

Traumatic Intracranial Bleeding Bleeding is a common complication of traumatic brain injury It is associated with poor outcome It can develop or worsen after hospital admission Early intervention may prevent enlargement Perel P, Roberts I, Bouamra O, Woodford M, Mooney J, Lecky F. Intracranial bleeding in patients with traumatic brain injury: A prognostic study. BMC Emergency Medicine 2009, 9:15 Oertel M, Kelly DF, McArthur D, Boscardin WJ, Glenn TC, Lee JH, et al. Progressive hemorrhage after head trauma: predictors and consequences of the evolving injury. J Neurosurg. 2002;96(1):109 16. Narayan RK, Maas AI, Servadei F, Skolnick BE, Tillinger MN, Marshall LF. Progression of traumatic intracerebral hemorrhage: aprospective observational study. J Neurotrauma. 2008; 25(6):629 39.

Tranexamic acid and Intracranial Bleeding Coagulopathy affects about one third of patients with TBI Increased fibrinolysis is a common feature of coagulopathy Two randomised controlled trials of TXA in TBI Harhangi BS, Kompanje EJ, Leebeek FW, Maas AI. Coagulation disorders after traumatic brain injury. Acta Neurochir (Wien). 2008;150(2):165 75. Bayir A, Kalkan E, Koçak S, Ak A, Cander B, Bodur S. Fibrinolytic markers and neurologic outcome in traumatic brain injury. Neurol India. 2006; 54(4):363 5.

Tranexamic acid and Intracranial Bleeding Significant haemorrhage growth (n 123/126) New focal ischaemic regions (n 123/126) TXA n (%) Placebo n (%) OR (95% CI) n=249 44 (36) 56 (44) 0.70 (0.42 1.16) 6 (5) 12 (9) 0.49 (0.18 1.35) Death (n 133/137) 14 (10.5) 24 (17.5) 0.55 (0.27 1.22) CRASH 2 collaborators (Intracranial Bleeding Study). Effect of tranexamic acid in traumatic brain injury: a nested randomised, placebo controlled trial (CRASH 2 Intracranial Bleeding Study). BMJ 2011; 343:d3795.

Tranexamic acid and Intracranial Bleeding 240 patients with isolated TBI RR (95% CI) Haemorrhage growth 0.56 (0.32 0.96) Mortality 0.67 (0.34 1.32) Yutthakasemsunt S, et al. Tranexamic Acid for preventing progressive intracranial hemorrage in adults with traumatic brain injury; a preliminary report presented at the National Neurotrauma Symposium 2010. Available from http://www.neurotrauma.org/2010/abstracts.htm

Meta analysis Significant Haemorrhage growth CRASH 2 IBS Thai study

Meta analysis Mortality CRASH 2 IBS Thai study

Randomised Placebo Controlled Clinical Trial The CRASH 3 trial will provide reliable evidence about the effect of tranexamic acid on mortality and disability in patients with TBI. The effect of TXA on the risk of vascular occlusive events and seizures will also be assessed.

Overview ELIGIBILITY adult with traumatic brain injury within 8 hours of injury any intracranial bleeding on CT scan OR GCS 12 no significant extracranial extra cranial haemorrhage where the responsible clinician is substantially uncertain as to the appropriateness of antifibrinolytic agents in a patient Appropriate CONSENT PROCESS for patient eg prior representative agreement or waiver RANDOMISE (tranexamic acid or placebo) Entry form completed Give loading dose over 10 minutes Give maintenance dose over 8 hours Complete outcome form at prior discharge, death, or day 28 All clinically indicated treatment is given in addition to trial enrolment Adverse events are reported up to day 28 If prior consent waiver used, consent from patient or representative required after emergency is over

Rationale for eligibility Adult Within 8 hours of injury Intracranial bleeding on CT scan OR GCS 12 Any intracranial bleeds included Uncertainty principle Why exclude CRASH 2 type patients?

Give trial treatment as soon as possible

Safety overview Data Monitoring Committee Primary outcome Death in hospital within four weeks of injury Secondary outcomes Vascular occlusive events MI, Stroke, PE, DVT Seizures Disability Other adverse events any AE and SAE

Deaths prevented each year giving TXA < 1 hour = 128,000 lives Deaths prevented each year giving TXA < 3 hours =112,000 lives Ker et al. BMC Emergency Medicine 2012, 12:3

Trial Coordinating Centre London School of Hygiene & Tropical Medicine Room 180, Keppel Street, London WC1E 7HT Tel +44(0)20 7299 4684 Fax +44(0)20 7299 4663 crash@lshtm.ac.uk crash3.lshtm.ac.uk