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MANAGEMENT OF
MASSIVE
BLOOD LOSS
Dr.Sripali Dassanayake
Massive blood loss
Jeopardise survival of patient
Doctors attempting to treat
bleeding
Blood bank
Laboratory
DISCORD-waste of resources
Bad outcome
Definition
MASSIVE BLOOD LOSS =
Loss of one blood volume within 24 hours
 ADULT-7% of ideal body weight
(70Kg;70*7/100=4.9l)
 CHILDREN-8%-9%
OR
Loss of 50% blood volume within 3 hours
OR a rate of loss of 150ml/min
Clinical situations
 Multiple trauma
 PPH
 Ruptured ectopic
 APH
 Injury to the highly vascular area; involving
lung,liver,spleen,prostate
 Any major Sx with prolonged exposure
 Any surgical or obstetric emergency
Priorities of Rx
1.Restoration of blood volume to maintain tissue
perfusion & oxygenation
2.Achieving haemostasis by;
Treating any traumatic, surgical or obstetric
source of bleeding
Correcting coagulopathy by the judicious use of
blood component therapy
OUTCOME
Early, Prompt action and Good
communication between clinical
specialities
Blood bank
staff
Local blood
centre
Diagnostic
laboratories
Surgical team
Haematological
team
Anaesthetic
team
Templated Guidelines updated
2008,March(R/V in July)
Goal Procedure Comment
Restore circulating volume Insert wide bore peripheral
cannulae
Give adequate volumes of
warmed crystalloids
? Colloids
Blood
Aim to maintain normal
blood pressure and urine
output-30ml/hr
14G or larger
MonitorCentralVenous Pressure
Blood loss is often
underestimated
Keep patient warm
Contact key personnel Clinician incharge
Duty anaesthetist
Blood bank
Duty haematologist
Nominated co-odinator should
take responsibility for
communication and
documentation
Goal Procedure Comment
Arrest bleeding Early surgical or obstetric
intervention
Interventional radiology
Request laboratory
investigations
FBC,PT,APTT,Thrombin
time, fibrinogen(Clauss
method);blood bank
sample, biochemical
profile, blood gases &
pulse oxymetry
Ensure correct sample
identity
Repeat
FBC,PT,APTT,Fibrinogen
4hrly or after 1/3 of blood
volume replacement
Repeat after blood
component infusion
Take samples at earliest opportunity
as results may be affected by colloid
infusion
Misidentification is the commonest
transfusion risk
May need to give components
before results available
Request suitable red cells
Maintain Hb>8g/dl
Assess degree of urgency
Un-crossmatched group O
Rh negative in extreme
emergency
No more than 2 units
Un-crossmatched ABO
group specific when blood
group is known
Fully cross-matched
When irregularAb present
When time permits
Use blood warmer and/or
rapid infusion device
Employ blood salvage if
available and appropriate to
minimize allogenic blood
use
Rh positive is acceptable if
patient is a male or
postmenopausal female
Laboratory will complete
crossmatch after issue
Further cross-match not
required after replacement
of one blood volume(8-10
units)
Blood warmer indicated if
flow rate>50ml/kg/hr in
adult
Salvage is contraindicated if
wound is contaminated.
Collection of split can be
setup in <10min.
Request platelets
Maintain platelets
>75,00o
Allow for delivery time from blood
centre
Anticipate platelet count <50,000
after 2* blood volume replacement
Target platelet count
100,000 for multiple /CNS
trauma or if platelet function
abnormal
>50,000 in other situations
Request FFP
(12-15ml/kg body
weight=1L or 4
units for an adult
<1u FFP=2-5mg
fibrinogen/ml>
Aim for PT &APTT<1.5*control
mean
Critical level is 1g/l
Anticipate need for FFP after 1-
1.5*blood volume replacement
Allow for ~30min thawing time
PT/APTT>1.5 of mean normal
value- correlates with
increased microvascular
bleeding
(<0.5 g/l of fibrinogen)
Keep ionizedCa+2
>1.13mmol/l
Maintain f
fibrinogen 1.0g/l
1.8g of fib/pool
If not corrected by FFP give
cryoprecipitate(2 packs of pooled
cryoprecipitate for an adult)
Should be available on side
Allow for 30min thawing time
Cryoprecipitate rarely needed
except in DIC
Suspect & Avoid
DIC
Treating underlying causes;
Shock
Hypothermia
acidosis
Although rare, mortality is
high
Use of pharmacological agents
to arrest bleeding
 Antifibrinolytic drugs
 Tranexamic acid reverse fibrinolysis
 Aprotinin
 Recombinant factor viia-for haemophyliacs
 Where blood loss is>300ml/hr
 Where no effects of heparin/warfarin
 Where surgical control of bleeding is not possible
 After adequate replacement of coagulation factor
with FFP,cryoprecipitate and platelets
 After correction of acidosis
Disseminated Intra vascular
Coagulation(DIC)
 Microvascular oozing-cardinal clinical sign
 Microthrombi in small vessels-end organ
damage
 DIC like syndrome:

Tissue trauma activation of coagulation
cascade
 Platelet +coagulation factor consumption
Patients at risk
 prolonged hypoxia
 Hypovolaemia
 Hypothermia
 Massive head injury
 Extensive muscle damage
High mortality=difficult to
reverse
 Appropriate and aggressive Rx needed before
microvascular bleeding is evident
based on laboratory evidence of consumption coagulopathy;
 Prolongation of PT/APTT (more than accepted levels by
dilution)
 Significant thrombocytopenia
 Fibrinogen levels<1g/l
 Measurement of D-dimers
 FFP and cryoprecipitate should be replaced “sooner rather
than later "in sufficient dosage avoiding circulatory
overload.
Risks of massive transfusion
1 .Giving the wrong blood to the pt.-most frequent & hazardous-must
adhere to the protocols in whatever degree of emergency
2 .Transfusion related acute lung injury (TRALI) –
*dyspnoea, fever & hypotension within hours of trnsfusion
*Potentially life threatening
3 . Acute immunological mediated reactions-Rare
BUT 5-6times frequent in platelet &FFP transfusion compared to red cell
transfusion
4 .Transfusion associated haemodilution-suppress immune response-risk of
post op infections
5 .Creutzfeldt-Jakob disease(vCJD):-rare, but invariably fatal
Metabolic consequences of
massive transfusion
1.Ionized hypocalcaemia due to citrate toxicity
1. - commonest : in large volumes of plasma infusion-
specially with abnormal liver functions(slowed
citrate metabolism)
 -reduces myocardial contractility, vasodilation-
exacerbate further bleeding & shock
*Measure Ca+2 –blood gas analyser
 Rx –IV CaCl2 infusion(not gluconate-needs liver
metabolism to release ionized Ca)
 Dose 10ml of 10% CaCl2 IV OR 2.5-5mmol CaCl2 in
divided doses over 10min.
 2.Hyperkalaemia
 -high extracellular K+ in stored red cell units-
compounded by oliguria & metabolic acidosis
associated with shock.
 If >6mmol/l glucose insulin regime +
 Bicarbonate(for acidosis)
In severe cases-haemofiltration
Patients survival
depends on:-
 **PROMPTACTION
 ***GOOD COMMUNICATION
 **INVOLVEMENT OF SENIOR CLINICIANS
WITH NECESSARY EXPERTISE
 **Better understanding of the associated
physiological changes
 More aggressive resuscitation
 Effective blood component therapy guided by
lab/near patient testing
 Effective warming techniques
 **PATIENT’SAGE & CO-MORBIDITY
 **DURATION & DEGREE OF SHOCK
 **DEVELOPMENTOF DIC
Any Questions……????
Management of massive blood loss

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Management of massive blood loss

  • 2. Massive blood loss Jeopardise survival of patient Doctors attempting to treat bleeding Blood bank Laboratory DISCORD-waste of resources Bad outcome
  • 3. Definition MASSIVE BLOOD LOSS = Loss of one blood volume within 24 hours  ADULT-7% of ideal body weight (70Kg;70*7/100=4.9l)  CHILDREN-8%-9% OR Loss of 50% blood volume within 3 hours OR a rate of loss of 150ml/min
  • 4. Clinical situations  Multiple trauma  PPH  Ruptured ectopic  APH  Injury to the highly vascular area; involving lung,liver,spleen,prostate  Any major Sx with prolonged exposure  Any surgical or obstetric emergency
  • 5. Priorities of Rx 1.Restoration of blood volume to maintain tissue perfusion & oxygenation 2.Achieving haemostasis by; Treating any traumatic, surgical or obstetric source of bleeding Correcting coagulopathy by the judicious use of blood component therapy
  • 6. OUTCOME Early, Prompt action and Good communication between clinical specialities Blood bank staff Local blood centre Diagnostic laboratories
  • 8. Templated Guidelines updated 2008,March(R/V in July) Goal Procedure Comment Restore circulating volume Insert wide bore peripheral cannulae Give adequate volumes of warmed crystalloids ? Colloids Blood Aim to maintain normal blood pressure and urine output-30ml/hr 14G or larger MonitorCentralVenous Pressure Blood loss is often underestimated Keep patient warm Contact key personnel Clinician incharge Duty anaesthetist Blood bank Duty haematologist Nominated co-odinator should take responsibility for communication and documentation
  • 9. Goal Procedure Comment Arrest bleeding Early surgical or obstetric intervention Interventional radiology Request laboratory investigations FBC,PT,APTT,Thrombin time, fibrinogen(Clauss method);blood bank sample, biochemical profile, blood gases & pulse oxymetry Ensure correct sample identity Repeat FBC,PT,APTT,Fibrinogen 4hrly or after 1/3 of blood volume replacement Repeat after blood component infusion Take samples at earliest opportunity as results may be affected by colloid infusion Misidentification is the commonest transfusion risk May need to give components before results available
  • 10. Request suitable red cells Maintain Hb>8g/dl Assess degree of urgency Un-crossmatched group O Rh negative in extreme emergency No more than 2 units Un-crossmatched ABO group specific when blood group is known Fully cross-matched When irregularAb present When time permits Use blood warmer and/or rapid infusion device Employ blood salvage if available and appropriate to minimize allogenic blood use Rh positive is acceptable if patient is a male or postmenopausal female Laboratory will complete crossmatch after issue Further cross-match not required after replacement of one blood volume(8-10 units) Blood warmer indicated if flow rate>50ml/kg/hr in adult Salvage is contraindicated if wound is contaminated. Collection of split can be setup in <10min.
  • 11. Request platelets Maintain platelets >75,00o Allow for delivery time from blood centre Anticipate platelet count <50,000 after 2* blood volume replacement Target platelet count 100,000 for multiple /CNS trauma or if platelet function abnormal >50,000 in other situations Request FFP (12-15ml/kg body weight=1L or 4 units for an adult <1u FFP=2-5mg fibrinogen/ml> Aim for PT &APTT<1.5*control mean Critical level is 1g/l Anticipate need for FFP after 1- 1.5*blood volume replacement Allow for ~30min thawing time PT/APTT>1.5 of mean normal value- correlates with increased microvascular bleeding (<0.5 g/l of fibrinogen) Keep ionizedCa+2 >1.13mmol/l Maintain f fibrinogen 1.0g/l 1.8g of fib/pool If not corrected by FFP give cryoprecipitate(2 packs of pooled cryoprecipitate for an adult) Should be available on side Allow for 30min thawing time Cryoprecipitate rarely needed except in DIC Suspect & Avoid DIC Treating underlying causes; Shock Hypothermia acidosis Although rare, mortality is high
  • 12. Use of pharmacological agents to arrest bleeding  Antifibrinolytic drugs  Tranexamic acid reverse fibrinolysis  Aprotinin  Recombinant factor viia-for haemophyliacs  Where blood loss is>300ml/hr  Where no effects of heparin/warfarin  Where surgical control of bleeding is not possible  After adequate replacement of coagulation factor with FFP,cryoprecipitate and platelets  After correction of acidosis
  • 13. Disseminated Intra vascular Coagulation(DIC)  Microvascular oozing-cardinal clinical sign  Microthrombi in small vessels-end organ damage  DIC like syndrome:  Tissue trauma activation of coagulation cascade  Platelet +coagulation factor consumption
  • 14. Patients at risk  prolonged hypoxia  Hypovolaemia  Hypothermia  Massive head injury  Extensive muscle damage
  • 15. High mortality=difficult to reverse  Appropriate and aggressive Rx needed before microvascular bleeding is evident based on laboratory evidence of consumption coagulopathy;  Prolongation of PT/APTT (more than accepted levels by dilution)  Significant thrombocytopenia  Fibrinogen levels<1g/l  Measurement of D-dimers  FFP and cryoprecipitate should be replaced “sooner rather than later "in sufficient dosage avoiding circulatory overload.
  • 16. Risks of massive transfusion 1 .Giving the wrong blood to the pt.-most frequent & hazardous-must adhere to the protocols in whatever degree of emergency 2 .Transfusion related acute lung injury (TRALI) – *dyspnoea, fever & hypotension within hours of trnsfusion *Potentially life threatening 3 . Acute immunological mediated reactions-Rare BUT 5-6times frequent in platelet &FFP transfusion compared to red cell transfusion 4 .Transfusion associated haemodilution-suppress immune response-risk of post op infections 5 .Creutzfeldt-Jakob disease(vCJD):-rare, but invariably fatal
  • 17. Metabolic consequences of massive transfusion 1.Ionized hypocalcaemia due to citrate toxicity 1. - commonest : in large volumes of plasma infusion- specially with abnormal liver functions(slowed citrate metabolism)  -reduces myocardial contractility, vasodilation- exacerbate further bleeding & shock *Measure Ca+2 –blood gas analyser  Rx –IV CaCl2 infusion(not gluconate-needs liver metabolism to release ionized Ca)  Dose 10ml of 10% CaCl2 IV OR 2.5-5mmol CaCl2 in divided doses over 10min.
  • 18.  2.Hyperkalaemia  -high extracellular K+ in stored red cell units- compounded by oliguria & metabolic acidosis associated with shock.  If >6mmol/l glucose insulin regime +  Bicarbonate(for acidosis) In severe cases-haemofiltration
  • 19. Patients survival depends on:-  **PROMPTACTION  ***GOOD COMMUNICATION  **INVOLVEMENT OF SENIOR CLINICIANS WITH NECESSARY EXPERTISE  **Better understanding of the associated physiological changes  More aggressive resuscitation  Effective blood component therapy guided by lab/near patient testing  Effective warming techniques
  • 20.  **PATIENT’SAGE & CO-MORBIDITY  **DURATION & DEGREE OF SHOCK  **DEVELOPMENTOF DIC