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Tranexamic acid safely reduces mortality
      in bleeding trauma patients

     Here we present the evidence
Millions bleed to death after trauma each year

There are millions of trauma deaths each year. Many
patients survive to reach hospital. This slide shows the
          causes of in-hospital trauma deaths


       Bleeding                        CNS injury
         45%                             41%




                  Other        Organ failure
                   4%              10%
Coagulation and Fibrinolysis


         In bleeding trauma patients:

          Coagulation occurs rapidly at the site of
           damaged blood vessels.

          Fibrinolysis breaks down blood clots.

          In patients with serious bleeding fibrinolysis
           can make bleeding worse.
Fibrinolysis


  Plasminogen activators from injured blood
   vessel convert plasminogen to plasmin.

  Plasmin binds to the fibrin blood clot and
   breaks it down. This is fibrinolysis.
Tranexamic acid reduces fibrinolysis


              Tranexamic acid inhibits plasmin and
               reduces clot breakdown.
Tranexamic acid reduces surgical bleeding
 In surgical patients tranexamic acid (TXA) reduces the
      need for blood transfusion by about one third.

                Need for transfusion

                         RR (95% CI)



                TXA            0.61 (0.54–0 .69)




                0.4      0.8      1.2      1.6
                 TXA better        TXA worse
The CRASH-2 Trial
   Tranexamic acid reduces clot breakdown

 Tranexamic acid reduces bleeding in surgery

   Many trauma patients die from bleeding

To see if tranexamic acid saves lives in bleeding
  trauma patients we conducted a very large
 Randomised Controlled Trial called CRASH-2
Methods

 Over 20,000 bleeding trauma patients were randomly
  allocated to get tranexamic acid or matching placebo

 We included all adult trauma patients who were
  within 8 hours of their injury, if their doctor thought
  that they had or could have significant haemorrhage

 We then collected data on death in hospital within
  4 weeks of injury and all important side effects
We used this dose of tranexamic acid

   Treatment           Tranexamic acid dose

                       1 gram over 10 minutes
    Loading     (by slow intravenous injection or an
                   isotonic intravenous infusion)

                         1 gram over 8 hours
  Maintenance
                (in an isotonic intravenous infusion)
We randomised many trauma patients

Patient enrolment
 20,211 patients


 from 274 hospitals


 in 40 countries
We had excellent follow up
               20,211 randomised


10,096 allocated TXA     10,115 allocated placebo

3 consent                              1 consent
withdrawn                              withdrawn



10,093 baseline data       10,114 baseline data

   33 lost                               47 lost
to follow-up                          to follow-up


Followed up = 10,060      Followed up = 10,067
      (99.7%)                   (99.5%)
Baseline factors were well balanced

                  TXA n (%)       Placebo n (%)
   Gender
    Male           8,439 (83.6)      8,496 (84.0)
    Female         1,654 (16.4)      1,617 (16.0)
    [not known]               0                1

   Age (years)
    <25            2,783 (27.6)      2,855 (28.2)
    25–34          3,012 (29.8)      3,081 (30.5)
    35–44          1,975 (19.6)      1,841 (18.2)
    >44            2,321 (23.0)      2,335 (23.1)
    [not known]               2                2
Baseline factors were well balanced

                               TXA n (%)       Placebo n (%)
   Time since injury (hours)
    ≤1 hour                     3,756 (37.2)      3,722 (36.8)
    >1 to ≤3 hours              3,045 (30.2)      3,006 (29.7)
    >3 hours                    3,006 (29.7)      3,380 (33.4)
    [not known]                            5                6

   Type of injury
    Blunt                       6,812 (67.5)      6,843 (67.7)
    Penetrating                 3,281 (32.5)      3,271 (32.3)
Baseline factors were well balanced

                           TXA n (%)        Placebo n (%)
   Systolic Blood Pressure (mmHg)
    >89                      6,901 (68.4)      6,791 (67.1)
    76–89                    1,615 (16.0)      1,697 (16.8)
    ≤75                      1,566 (15.5)      1,608 (15.9)
    [not known]                       11                18

   Glasgow Coma Score
    Severe (3–8)             1,799 (17.8)      1,839 (18.2)
    Moderate (9–12)          1,353 (13.4)      1,351 (13.4)
    Mild (13–15)             6,934 (68.7)      6,908 (68.3)
    [not known]                        7                16
This is what we found
Cause of death      TXA    Placebo   Risk of death      P value
                    10,060 10,067

Bleeding            489    574       0.85 (0.76–0.96)   0.0077

Thrombosis          33     48        0.69 (0.44–1.07)   0.096

Organ failure       209    233       0.90 (0.75–1.08)    0.25

Head injury         603    621       0.97 (0.87–1.08)    0.60

Other               129    137       0.94 (0.74–1.20)    0.63

Any death          1463    1613      0.91 (0.85–0·97)   0·0035
Most of the benefit is for bleeding deaths


    TXA (n= 10,060)            Placebo (n= 10,067)      RR (95% CI)
    489 (4.9%)                 574 (5.7%)




  0.85 (0.76–0.96) 2P=0.0077



                                0.8           0.9           1.0          1.1
                                               TXA better         TXA worse
For bleeding deaths – early treatment is better

                                 RR (99% CI)     p=0.000008




≤1 hour                                                              0.68 (0.54–0.86)


>1 to ≤ 3 hours                                                      0.79 (0.60–1.04)


>3 hours                                                             1.44 (1.04–1.99)

                                       0.85 (0.76–0.96)

                  .7   .8   .9     1     1.1   1.2   1.3   1.4 1.5
Treatment must be given early because
bleeding deaths happen soon after injury
                    1200




                    1000

                                                                   Deaths due to all other causes
 Number of deaths




                     800
                                                                   Deaths due to bleeding
                     600




                     400




                     200




                       0

                           0 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28
                                                              Days
There was no increase in thrombosis
         TXA         Placebo
         allocated   allocated
         (10,060)    (10,067)                       Risk ratio (95% CI)



DVT      40 (0.40%) 41 (0.41%)

PE       72 (0.69%) 71 (0.70%)

MI       35 (0.35%) 55 (0.52%)

Stroke   57 (0.56%) 66 (0.65%)

Any      168 (1.63%) 201 (1.95%)

                                   .6   .7   .8     .9         1   1.1    1.2
                                                  TXA better         TXA worse
Tranexamic acid reduces symptoms
                       TXA           Placebo
                                                      RR (95% CI)       p-value
                    [n=10060]       [n=10067]
No symptoms        1,483 (17.3%)   1,334 (15.8%)   1.11 (1.04 – 1.19) 0.0023

Minor symptoms     3,054 (30.4%)   3,061 (30.4%)   1.00 (0.96 – 1.04)    0.94

Some restriction   2,016 (20.0%)   2,069 (20.6%)   0.97 (0.92 – 1.03)    0.36

Dependent          1,294 (12.9%)   1,273 (12.6%)   1.02 (0.95 – 1.09)    0.63

Fully dependent     696 (6.9%)      676 (6.7%)     1.03 (0.93 – 1.14)    0.57

Dead               1,463 (14.5%)   1,613 (16.0%)   0.91 (0.85 – 0.97) 0.0035
CRASH-2 was conducted on 4 continents and...




   was shown to reduce mortality on each!
Tranexamic acid is highly cost effective
What we concluded
 Tranexamic acid reduces mortality in bleeding trauma patients

 Tranexamic acid does not seem to increase unwanted clotting

 Tranexamic acid needs to be given early – within 3 hours of
  injury

 Tranexamic acid is not expensive and could save hundreds of
  thousands of lives each year around the world
Tranexamic acid is now being used
 After the CRASH-2 trial, tranexamic acid was added to the
  WHO List of Essential Medicines (March 2011)

 The military are using tranexamic acid to treat combat
  casualties

 Tranexamic acid is being used in hospitals around the world


 Tranexamic acid could be given in ambulances

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Tx ain trauma_english

  • 1. Tranexamic acid safely reduces mortality in bleeding trauma patients Here we present the evidence
  • 2. Millions bleed to death after trauma each year There are millions of trauma deaths each year. Many patients survive to reach hospital. This slide shows the causes of in-hospital trauma deaths Bleeding CNS injury 45% 41% Other Organ failure 4% 10%
  • 3. Coagulation and Fibrinolysis In bleeding trauma patients:  Coagulation occurs rapidly at the site of damaged blood vessels.  Fibrinolysis breaks down blood clots.  In patients with serious bleeding fibrinolysis can make bleeding worse.
  • 4. Fibrinolysis  Plasminogen activators from injured blood vessel convert plasminogen to plasmin.  Plasmin binds to the fibrin blood clot and breaks it down. This is fibrinolysis.
  • 5. Tranexamic acid reduces fibrinolysis  Tranexamic acid inhibits plasmin and reduces clot breakdown.
  • 6. Tranexamic acid reduces surgical bleeding In surgical patients tranexamic acid (TXA) reduces the need for blood transfusion by about one third. Need for transfusion RR (95% CI) TXA 0.61 (0.54–0 .69) 0.4 0.8 1.2 1.6 TXA better TXA worse
  • 7. The CRASH-2 Trial Tranexamic acid reduces clot breakdown Tranexamic acid reduces bleeding in surgery Many trauma patients die from bleeding To see if tranexamic acid saves lives in bleeding trauma patients we conducted a very large Randomised Controlled Trial called CRASH-2
  • 8. Methods  Over 20,000 bleeding trauma patients were randomly allocated to get tranexamic acid or matching placebo  We included all adult trauma patients who were within 8 hours of their injury, if their doctor thought that they had or could have significant haemorrhage  We then collected data on death in hospital within 4 weeks of injury and all important side effects
  • 9.
  • 10. We used this dose of tranexamic acid Treatment Tranexamic acid dose 1 gram over 10 minutes Loading (by slow intravenous injection or an isotonic intravenous infusion) 1 gram over 8 hours Maintenance (in an isotonic intravenous infusion)
  • 11. We randomised many trauma patients Patient enrolment  20,211 patients  from 274 hospitals  in 40 countries
  • 12. We had excellent follow up 20,211 randomised 10,096 allocated TXA 10,115 allocated placebo 3 consent 1 consent withdrawn withdrawn 10,093 baseline data 10,114 baseline data 33 lost 47 lost to follow-up to follow-up Followed up = 10,060 Followed up = 10,067 (99.7%) (99.5%)
  • 13. Baseline factors were well balanced TXA n (%) Placebo n (%) Gender Male 8,439 (83.6) 8,496 (84.0) Female 1,654 (16.4) 1,617 (16.0) [not known] 0 1 Age (years) <25 2,783 (27.6) 2,855 (28.2) 25–34 3,012 (29.8) 3,081 (30.5) 35–44 1,975 (19.6) 1,841 (18.2) >44 2,321 (23.0) 2,335 (23.1) [not known] 2 2
  • 14. Baseline factors were well balanced TXA n (%) Placebo n (%) Time since injury (hours) ≤1 hour 3,756 (37.2) 3,722 (36.8) >1 to ≤3 hours 3,045 (30.2) 3,006 (29.7) >3 hours 3,006 (29.7) 3,380 (33.4) [not known] 5 6 Type of injury Blunt 6,812 (67.5) 6,843 (67.7) Penetrating 3,281 (32.5) 3,271 (32.3)
  • 15. Baseline factors were well balanced TXA n (%) Placebo n (%) Systolic Blood Pressure (mmHg) >89 6,901 (68.4) 6,791 (67.1) 76–89 1,615 (16.0) 1,697 (16.8) ≤75 1,566 (15.5) 1,608 (15.9) [not known] 11 18 Glasgow Coma Score Severe (3–8) 1,799 (17.8) 1,839 (18.2) Moderate (9–12) 1,353 (13.4) 1,351 (13.4) Mild (13–15) 6,934 (68.7) 6,908 (68.3) [not known] 7 16
  • 16. This is what we found Cause of death TXA Placebo Risk of death P value 10,060 10,067 Bleeding 489 574 0.85 (0.76–0.96) 0.0077 Thrombosis 33 48 0.69 (0.44–1.07) 0.096 Organ failure 209 233 0.90 (0.75–1.08) 0.25 Head injury 603 621 0.97 (0.87–1.08) 0.60 Other 129 137 0.94 (0.74–1.20) 0.63 Any death 1463 1613 0.91 (0.85–0·97) 0·0035
  • 17. Most of the benefit is for bleeding deaths TXA (n= 10,060) Placebo (n= 10,067) RR (95% CI) 489 (4.9%) 574 (5.7%) 0.85 (0.76–0.96) 2P=0.0077 0.8 0.9 1.0 1.1 TXA better TXA worse
  • 18. For bleeding deaths – early treatment is better RR (99% CI) p=0.000008 ≤1 hour 0.68 (0.54–0.86) >1 to ≤ 3 hours 0.79 (0.60–1.04) >3 hours 1.44 (1.04–1.99) 0.85 (0.76–0.96) .7 .8 .9 1 1.1 1.2 1.3 1.4 1.5
  • 19. Treatment must be given early because bleeding deaths happen soon after injury 1200 1000 Deaths due to all other causes Number of deaths 800 Deaths due to bleeding 600 400 200 0 0 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 Days
  • 20. There was no increase in thrombosis TXA Placebo allocated allocated (10,060) (10,067) Risk ratio (95% CI) DVT 40 (0.40%) 41 (0.41%) PE 72 (0.69%) 71 (0.70%) MI 35 (0.35%) 55 (0.52%) Stroke 57 (0.56%) 66 (0.65%) Any 168 (1.63%) 201 (1.95%) .6 .7 .8 .9 1 1.1 1.2 TXA better TXA worse
  • 21. Tranexamic acid reduces symptoms TXA Placebo RR (95% CI) p-value [n=10060] [n=10067] No symptoms 1,483 (17.3%) 1,334 (15.8%) 1.11 (1.04 – 1.19) 0.0023 Minor symptoms 3,054 (30.4%) 3,061 (30.4%) 1.00 (0.96 – 1.04) 0.94 Some restriction 2,016 (20.0%) 2,069 (20.6%) 0.97 (0.92 – 1.03) 0.36 Dependent 1,294 (12.9%) 1,273 (12.6%) 1.02 (0.95 – 1.09) 0.63 Fully dependent 696 (6.9%) 676 (6.7%) 1.03 (0.93 – 1.14) 0.57 Dead 1,463 (14.5%) 1,613 (16.0%) 0.91 (0.85 – 0.97) 0.0035
  • 22. CRASH-2 was conducted on 4 continents and... was shown to reduce mortality on each!
  • 23. Tranexamic acid is highly cost effective
  • 24. What we concluded  Tranexamic acid reduces mortality in bleeding trauma patients  Tranexamic acid does not seem to increase unwanted clotting  Tranexamic acid needs to be given early – within 3 hours of injury  Tranexamic acid is not expensive and could save hundreds of thousands of lives each year around the world
  • 25. Tranexamic acid is now being used  After the CRASH-2 trial, tranexamic acid was added to the WHO List of Essential Medicines (March 2011)  The military are using tranexamic acid to treat combat casualties  Tranexamic acid is being used in hospitals around the world  Tranexamic acid could be given in ambulances