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Blood transfusion

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Aashissh Shah

This document discusses blood transfusion, including definitions, types of transfusions, blood products, indications for transfusion, risks, and guidelines. It covers topics like whole blood, packed red blood cells, platelets, plasma, and cryoprecipitate. Key points include that transfusion involves receiving blood products intravenously to replace lost blood, it can use one's own blood or from a donor, and decisions should be based on careful assessment of clinical and lab indications to save life or prevent morbidity.

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introduction •BLOOD TRANSFUSION IS DEFINED AS THE PROCESS OF RECEIVING BLOOD PRODUCTS INTO ONE’S CIRCULATION INTRAVENOUSLY. THIS IS USUALLY DONE AS A LIFE SAVING MANEUVER TO REPLACE BLOOD CELLS OR BLOOD PRODUCTS LOST THROUGH SEVERE BLEEDING, DURING SURGERY WHEN SEVERE BLOOD LOSS OCCURS OR TO INCREASE THE BLOOD COUNT IN AN ANAEMIC PATIENT. •TRANSFUSIONS USUALLY INVOLVE THE USE OF TWO SOURCES OF BLOOD – ONE’S OWN (AUTOLOGOUS TRANSFUSION) OR SOMEONE ELSE’S (ALLOGENIC TRANSFUSION). •BLOOD TRANSFUSIONS INVOLVES THE USE OF WHOLE BLOOD , RED BLOOD CELLS, WHITE BLOOD CELLS, PLASMA, CLOTTING FACTORS AND PLATELETS.
Blood and blood products •BLOOD IS COLLECTED FROM DONORS WHO HAVE BEEN PREVIOUSLY SCREENED TO EXCLUDE ANY BLOOD OR BLOOD PRODUCTS THAT MAY HAVE THE POTENTIAL TO HARM THE PATIENT. •EACH UNIT OF BLOOD IS TESTED FOR EVIDENCE OF HEPATITIS-B, HEPATITIS-C , HUMAN IMMUNODEFICIENCY VIRUS I & II AND SYPHILIS. •THE ABO AND RHESUS D BLOOD GROUP IS DETERMINED AS WELL AS THE PRESENCE OF IRREGULAR RED CELL ANTIBODIES. •THE BLOOD IS THEN PROCESSED INTO SUB-COMPONENTS.
WHOLE BLOOD •WHOLE BLOOD IS UNSEPARATED BLOOD CONTAINING AN ANTICOAGULANT –PRESERVATIVE SOLUTION. ONE UNIT OF WHOLE BLOOD CONTAINS - • 450 ml OF DONOR BLOOD. • 50 ml OF ANTICOAGULANT-PRESERVATIVE SOLUTION. • HAEMOGLOBIN approx. 12g/ml & HAEMATOCRIT 35% - 45%. • NO FUNCTIONAL PLATELETS. •SINCE IT IS NOT STERILIZED, CAPABLE OF TRANSMITTING ANY AGENT PRESENT IN CELLS OR PLASMA WHICH HAS NOT BEEN DETECTED BY ROUTINE SCREENING. •HOWEVER WHOLE BLOOD TRANSFUSION HAS SIGNIFICANT ADVANTAGES OVER PACKED CELLS AS IT IS COAGULATION FACTOR RICH AND IF FRESH, MORE METABOLICALLY ACTIVE THAN STORED BLOOD.
• STORED BETWEEN +2 AND +6 DEGREES CENTIGRATE IN A BLOOD BANK REFRIGERATOR. •TRANSFUSION SHOULD BE STARTED WITHIN 30 MINUTES OF REMOVAL FROM THE REFRIGERATOR AND COMPLETED WITHIN 4 HOURS OF COMMENCEMENT BECAUSE CHANGES IN THE COMPOSITION MAY OCCUR DUE TO RED CELL METABOLISM. INDICATIONS – •RED CELL REPLACEMENT IN ACUTE BLOOD LOSS WITH HYPOVOLAEMIA •EXCHANGE TRANSFUSION CONTRAINDICATIONS – •CHRONIC ANAEMIA •INCIPIENT CARDIAC FAILURE
PACKED RED CELLS •PACKED RED CELLS ARE CELLS THAT ARE SPUN DOWN AND CONCENTRATED. •ONE UNIT OF PACKED RED CELLS IS APPROX. 330 ml AND HAS A HAEMATOCRIT OF 50-70%. •THEY ARE STORED IN A SAG-M (SALINE-ADENINE-GLUCOSE- MANNITOL) SOLUTION TO INCREASE THEIR SHELF LIFE TO 5 WEEKS AT 2-6 DEGREES CENTIGRATE. •IT CARRIES THE SAME INFECTION RISK AS IN WHOLE BLOOD. •INDICATED IN REPLACEMENT OF RED CELLS IN ANAEMIC PATIENTS AND ALSO USED WITH CRYSTALLOID AND COLLOID SOLUTIONS IN ACUTE BLOOD LOSS CONDITIONS.
FRESH FROZEN PLASMA •FRESH FROZEN PLASMA IS RICH IN COAGULATION FACTORS. •IT IS SEPARATED FROM WHOLE BLOOD AND STORED AT -40 TO -50 DEGREES CENTIGRATE WITH A 2 YEAR SHELF-LIFE. •IT IS THE FIRST LINE THERAPY IN THE TREATMENT OF COAGULOPATHIC HAEMORRHAGE. •ALSO USED IN THE REPLACEMENT OF MULTIPLE COAGULATION FACTOR DEFICIENCIES LIKE LIVER DISEASE, WARFARIN OVERDOSE, DEPLETION OF COAGULATION FACTORS IN PATIENTS RECEIVING LARGE VOLUME TRANSFUSIONS, DISSEMINATED INTRAVASULAR COAGULATION AND THROMBOTIC THROMBOCYTOPENIC PURPURA.
PRECAUTIONS – •ACUTE ALLERGIC REACTIONS ARE COMMON •SEVERE LIFE THREATENING ANAPHYLACTIC REACTIONS OCCASSIONALLY OCCUR. •DOSAGE – INITIAL DOSE OF 15ml/Kg.
Platelets •PLATELETS ARE SUPPLIED AS A POOLED PLATELET CONCENTRATE CONTAINING ABOUT 250 X 10 9 CELLS PER LITRE. •PLATELETS ARE STORED ON A SPECIAL AGITATOR AND HAVE A SHELF LIFE OF ONLY 5 DAYS. •ARE USUALLY GIVEN TO PATIENTS WITH THROMBOCYTOPENIA OR THOSE WITH PLATELET DYSFUNCTION WHO ARE BLEEDING OR UNDERGOING SURGERY AND IN PATIENTS WITH BONE MARROW FAILURE. •NOT INDICATED IN – • PATIENTS WITH ITP, TTP, UNTREATED DIC AND IN CASES OF HYPERSPLENISM.
•DOSAGE – 1 UNIT OF PLATELET CONCENTRATE /10 kg BODY WEIGHT. •4-6 DONOR UNITS OF PLATELET CONCENTRATES WILL RAISE THE PLATELET COUNT BY 20-40 X 109/L. INCREMENT WILL BE LESS IF THERE IS ASSOCIATED SEPTICEMIA, DIC, SPLENOMEGALY. •COMPLICATION S– FEBRILE AND ALLERGIC URTICARIAL REACTIONS ARE COMMON ESPECIALLY IN PATIENTS RECEIVING MULTIPLE TRANSFUSIONS. • PATIENTS ON ASPIRIN THERAPY RARLELY POSE A PROBLEM BUT THOSE PATIENTS ON CLOPIDOGREL WHO ARE ACTIVELY BLEEDING AND UNDERGOING MAJOR SURGERY MUST BE GIVEN A CONTINUOUS INFUSION DURING THE COURSE OF THE PROCEDURE.
CRYOPRECIPITATE •CRYOPRECIPITATE IS A SUPERNATANT PRECIPITATE OF FRESH FROZEN PLASMA AND IS RICH IN FACTOR VIII AND FIBRINOGEN. •IT IS STORED AT -30 DEGREES CENTIGRATE WITH A 2 YEARS SHELF LIFE. •INDICATED IN LOW FIBRINOGEN STATES (<1g/L) OR IN CASES OF FACTOR VIII DEFICIENCY (HAEMOPHILIA-A), VON WILLEBRAND’S DISEASE AND AS A SOURCE OF FIBRINOGEN IN DISSEMINATED INTRAVASCULAR COAGULATION. •POOLED UNITS CONTAINING 3-6 gms FIBRINOGEN IN 200-500 ml RAISES THE FIBRINOGEN LEVEL BY APPROX. 1g/L. •MUST BE INFUSED WITHIN 6 HOURS.
BLOOD GROUPS AND CROSS-MATCHING •HUMAN RED BLOOD CELLS HAVE MANY DIFFERENT ANTIGENS ON THEIR CELL SURFACE. •TWO GROUPS OF ANTIGENS ARE OF MAJOR IMPORTANCE IN MEDICAL PRACTICE – THE ABO AND THE RHESUS SYSTEMS. •ABO SYSTEM-THESE ARE STRONGLY ANTIGENIC AND ARE ASSOCIATED WITH NATURALLY OCCURING ANTIBODIES IN THE SERUM.THIS SYSTEM CONSISTS OF 3 ALLELIC GENES A,B & O. •GROUP A & B CONTAIN SPECIFIC ANTIGENS AND PROVOKE A REACTION IF THESE ANTIGENS ARE NOT PRESENT IN THE RECIPIENT. •GROUP ‘O’ CONTAINS NO ANTIGENS TO PROVOKE A REACTION IN THE RECIPIENT AND HENCE CALLED ‘AMORPHS’.
•THEREFORE, BLOOD GROUP ‘O’ IS CONSIDERED AS THE UNIVERSAL DONOR AS IT HAS NO ANTIGENS TO PROVOKE A REACTION AND ‘AB’ BLOOD TYPE IS CONSIDERED AS THE UNIVERSAL RECIPIENTS AS THEY HAVE NO CIRCULATING ANTIBODIES TO THEM. •RHESUS SYSTEM- THE RHESUS D ANTIGEN IS STRONGLY ANTIGENIC AND IS PRESENT IN APPROXIMATELY 85% OF THE POPULATION. ANTIBODIES TO THE ‘D’ ANTIGEN ARE NATURALLY NOT PRESENT IN THE REMAINING 15% OF THE INDIVIDUALS BUT THEIR FORMATION MAY BE STIMULATED BY THE TRANSFUSION OF RH’+’ RED CELLS OR THEY MAY BE ACQUIRED DURING DELIVERY OF A RH-D-POSITIVE BABY LEADING TO HAEMOLYTIC DISEASE OF THE NEWBORN IN A SUBSEQUENT PREGNANCY.
MAKING THE DECISION FOR BLOOD TRANSFUSION
•IF USED CORRECTLY, BLOOD TRANSFUSION CAN BE LIFE-SAVING, INAPPROPRIATE USE CAN ENDANGER LIFE. •THE DECISION TO TRANSFUSE BLOOD OR BLOOD PRODUCTS SHOULD ALWAYS BE BASED ON A CAREFUL ASSESSMENT OF CLINICAL AND LABORATORY INDICATIONS THAT TRANFUSION IS NECESSARY TO SAVE LIFE OR PREVENT SIGNIFICANT MORBIDITY.
minimising the need for blood transfusion •Preoperative planning- •History and examination including surgical or bleeding history •Full blood count, blood chemistry, coagulation, •Consider autologous blood deposit •Consider erythropoietin to boost haemoglobin concentration •Treat iron or folate deficiency •Stop aspirin prophylaxis if possible •Day of admission •Check if taking aspirin, non-steroidal anti-inflammatory drugs, anticoagulants •Repeat full blood count •Consider drugs to reduce bleeding (such as aprotinin)
During surgery •Be prepared for longer duration to secure haemostasis •Consider hypotensive surgery if appropriate •Avoid hypothermia—give all fluids through a warmer •Consider fibrin glues and sealants Postoperative care •Accept lower postoperative haemoglobin concentration •Accept transfusions of just one unit of blood, to exceed transfusion trigger •Use continuous face mask oxygen if patient has low haemoglobin concentration •Prescribe iron and folic acid routinely •Consider Tranexamic acid
•EXTERNAL BLEEDING & MEDICAL CONDITIONS LIKE THALASSEMIA. •INTERNAL BLEEDING –Eg. VARICEAL BLEEDING,ECTOPIC PREGNANCY, ANTEPARTUM HAEMORRHAGE , RUPTURED UTERUS, TRAUMATIC INJURIES TO THE CHEST, SPLEEN, PELVIS, LUNGS, RED CELL DESTRUCTION AS IN MALARIA, SEPSIS, DISSEMINATED INTRAVASCULAR COAGULATION. •CARDIORESPIRATORY STATE AND TISSUE OXYGENATION – BP, PULSE, RESPIRATORY RATE, CAPILLARY REFILL TIME, PERIPHERAL PULSES, TEMPERATURE, URINE OUTPUT, CARDIAC FAILURE. •ASSESSMENT OF ANAEMIA – CLINICALLY FROM THE TONGUE, PALMS, EYES, NAILS AND FROM LABORATORY ASSESSMENT OF THE HAEMOGLOBIN LEVEL OR HAEMATOCRIT. •ANTICIPATED SURGERY WHERE POST-OPERATIVE BLOOD LOSS IS HIGHLY PROBABLE , CONTINUOUS BLEEDING OR LIKELIHOOD OF RECURRENCE OF BLEEDING, CONTINUING HAEMOLYSIS.
CAUSES OF ACUTE BLOOD LOSS IN AN OBSTETRIC PATIENT •FETAL LOSS IN PREGNANCY – INCOMPLETE ABORTION, SEPTIC ABORTION. •ECTOPIC PREGNANCY – TUBAL, ABDOMINAL. •ANTEPARTUM HAEMORRHAGE – PLACENTA PREVIA, ABRUPTIO PLACENTAE, RUPTURED UTERUS, VASA PRAEVIA. •TRAUMATIC LESIONS – EPISIOTOMY, PERINEAL OR CERVICAL LACERATIONS, RUPTURED UTERUS. •POST-PARTUM HAEMORRHAGE – UTERINE ATONY, RETAINED PRODUCTS OF CONCEPTION, TRAUMATIC LESIONS, PUERPERAL SEPSIS, TISSUE DAMAGE FOLLOWING OBSTRUCTED LABOUR, BREAKDOWN OF UTERINE WOUND AFTER CAESAREAN SECTION. •DISSEMINATED INTRAVASCULAR COAGULATION INDUCED BY – IUFD, AMNIOTIC FLUID EMBOLISM, PRE-ECLAMPSIA, ABRUPTIO PLACENTAE, INDUCED ABORTION, RETAINED PRODUCTS OF CONCEPTION.
PERI-OPERATIVE RED BLOOD CELL TRANSFUSION CRITERIA HAEMOGLOBIN INDICATION LEVEL g/dl <6 Probably will benefit from transfusion 6-8 Transfusion unlikely to be of benefit in the absence of bleeding or impending surgery >8 No indication for transfusion
Who Transfusion guidelines for chronic anaemia during pregnancy DURATION OF PREGNANCY HAEMOGLOBIN LEVEL CONSIDER IF- <36 WEEKS 5.0 g/dl or LESS EVEN Hb 5.0-7.0g/dl + Established WITHOUT CLINICAL SIGNS or incipient cardiac failure, OF CARDIAC FAILURE OR Clinical evidence of hypoxia, HYPOXIA Pneumonia or any serious bacterial infections, Pre- existing heart disease. >36 WEEKS 6.0 g/dl OR LESS Hb 6.0 – 8.0 g/dl + Above mentioned conditions ELECTIVE CAESAREAN 8.0-10.0 g/dl- Confirm blood Elective CS Planned + SECTION group, Save freshly taken History of APH, PPH, serum for cross-matching. Previous CS. <8.0 g/dl – 2 Units of blood should be cross-matched and available.
ESTIMATING BLOOD LOSS •IN ORDER TO MAINTAIN BLOOD VOLUME ACCURATELY, IT IS ESSENTIAL TO CONTINUALLY ASSESS SURGICAL BLOOD LOSS THROUGHOUT THE PROCEDURE. BLOOD VOLUME NEONATES 85-90ml/kg Body Weight CHILDREN 80ml/kg Body Weight ADULTS 70ml/kg Body Weight Example: An adult weighing 60 kgs would have a blood volume equal to 70x60, which is 4200 ml. 1. Weigh swabs while still in their dry state. 2. Weigh the blood soaked swabs as soon as they are discarded and subtract their dry weight (1ml of blood weighs approximately 1 gm). 3. Weigh the ungraduated drains or suction bottles and subtract their empty weight.
4. Estimate blood loss into surgical drapes, together with that pooling beneath the patient and onto the floor. 5. Note the volume of any irrigation or wash out fluids that are used during surgery. Subtract this volume from the measured blood loss to arrive at a final estimate. • IN POST-OPERATIVE TRANSFUSION CASES, THE HAEMOGLOBIN LEVEL, URINE OUTPUT, BLOOD PRESSURE, PULSE RATE, HEART RATE, CAPILLARY REFILL TIME, COLOUR OF MUCOUS MEMBRANES, RESPIRATORY RATE AND SYMPTOMS AND SIGNS OF HYPOXIA SHOULD BE CAREFULLY MONITORED.
WHO ACCEPTABLE BLOOD LOSS GUIDELINE METHOD HEALTHY PATIENT AVERAGE CLINICAL POOR CLINICAL CONDITION CONDITION PERCENTAGE METHOD – 30% 20% <10% Acceptable loss of blood volume HAEMODILUTION METHOD – Lowest 9g/dl or 10g/dl or 11g/dl or acceptable Haematocrit Haematocrit Haematocrit Haemoglobin or Haematocrit = 27% = 30% =33% During surgery, however the decision to transfuse will ultimately need to be based on the careful assessment of Volume of blood loss, Rate of blood loss, Patient’s clinical response to blood loss and fluid replacement therapy & signs indicating inadequate tissue oxygenation.
SAFE BLOOD TRANSFUSION PROCEDURES
• EVERY HOSPITAL SHOULD HAVE WRITTEN STANDARD OPERATING PROCEDURES FOR THE ADMINISTRATION OF BLOOD PRODUCTS LIKE THE ONE WE HAVE IN OUR HOSPITAL , PARTICULARLY FOR THE FINAL IDENTITY CHECK OF THE PATIENT, THE COMPATIBILITY LABEL DETERMINING THE PATIENT’S ABO AND RH-D GROUP, UNIQUE DONATION NUMBER OF THE BLOOD PACK, BLOOD GROUP OF THE BLOOD PACK, THE DATE OF COLLECTION AND THE EXPIRY DATE, THE INDICATION FOR TRANSFUSION, SIGNATURE OF THE CLINICIAN PERFORMING THE PRE-TRANSFUSION IDENTITY CHECK AND THE TRANSDUSION PROCEDURE •THE BLOOD PACK SHOULD ALWAYS BE INSPECTED FOR SIGNS OF DETERIORATION ON ARRIVAL AND BEFORE TRANSFUSION IF NOT USED IMMEDIATELY. •DISCOLOURATION OF THE BLOOD PACK AND ANY SIGNS OF LEAKAGE INDICATE CONTAMINATION AND COULD CAUSE A SEVERE FATAL REACTION IF TRANSFUSED.
DISPOSABLE EQUIPMENT FOR BLOOD ADMINISTRATION • CANNULAS MUST BE STERILE AND MUST NEVER BE REUSED. • FLEXIBLE PLASTIC CANNULAS SHOULD BE USED AS THEY ARE SAFER AND PRESERVE THE VEINS. FOR WHOLE BLOOD, RED CELLS, PLASMA & CRYOPRECIPITATE •USE A NEW STERILE BLOOD ADMINISTRATION SET CONTAINING AN INTEGRAL 170-200 micron FILTER • CHANGE THE SET AT LEAST 12 HOURLY DURING BLOOD COMPONENT INFUSION. • IN A WARM CLIMATE, CHANGE THE SET MORE FREQUENTLY AND USUALLY AFTER EVERY 4 UNITS OF BLOOD IF GIVEN WITHIN A 12 HOUR PERIOD.
• THERE IS NO EVIDENCE THAT WARMING BLOOD IS BENEFICIAL TO THE PATIENT WHEN INFUSION IS SLOW. AT INFUSION RATES >100ml/minute, COLD BLOOD MAY BE A CONTRIBUTING FACTOR IN CARDIAC ARREST. HOWEVER, KEEPING THE PATIENT WARM IS PROBABLY MORE IMPORTANT THAN WARMING THE INFUSED BLOOD ! • WARMED BLOOD IS MOST COMMONLY REQUIRED IN LARGE VOLUME RAPID TRANSFUSIONS & EXCHANGE TRANSFUSION IN INFANTS. •BLOOD SHOULD ONLY BE WARMED IN A BLOOD WARMER THAT HAVE A VISIBLE THERMOMETER AND AN AUDIBLE WARNING ALARM AND SHOULD BE PROPERLY MAINTAINED.
INTRAVENOUS CANNULATIONS FOR BLOOD TRANSFUSION CAN BE DONE FROM – • CEPHALIC VEIN • BASILIC VEIN • FOREARM VEINS • GREAT SAPHENOUS VEINS
MONITORING THE TRANSFUSED PATIENT 1. FOR EACH UNIT OF BLOOD TRANSFUSED, MONITOR THE PATIENT: • BEFORE STARTING THE TRANSFUSION • 15 MINUTES AFTER STARTING THE TRANSFUSION • AT LEAST EVERY HOUR DURING TRANSFUSION • ON COMPLETION OF THE TRANSFUSION • 4 HOURS AFTER COMPLETING THE TRANSFUSION 2. AT EACH OF THESE STAGES, RECORD: • PATIENT’S GENERAL APPEARANCE • BLOOD PRESSURE, PULSE, RESPIRATORY RATE • FLUID BALANCE – ORAL AND IV FLUID INTAKE & URINARY OUTPUT.
3. RECORD: • TIME WHEN THE TRANSFUSION IS STARTED. • TIME WHEN THE TRANSFUSION IN COMPLETED. • VOLUME AND TYPE OF ALL PRODUCTS TRANSFUSED. • BLOOD PACK NUMBERS. • ANY ADVERSE EFFECTS. SEVERE REACTIONS MOST COMMONLY PRESENT IN THE FIRST 15-30 MINUTES OF A TRANSFUSION THEREFORE THEY SHOULD BE CLOSELY MONITORED DURING THIS TIME. IF THE PATIENT APPEARS TO BE EXPERIENCING AN ADVERSE REACTION THE TRANSFUSION MUST BE IMMEDIATELY STOPPED AND URGENT MEDICAL ASSISTANCE SHOULD BE SEEKED FOR.
REFERENCES: • the who handbook on the clinical use of blood – who blood transfusion safety , geneva , 2007. • bailey & love’s short practice of surgery – 25th edition – 2008. • davidson’s principle & practice of medicine – 21st edition – 2010. • essential paediatrics – o.p. ghai – 6th edition. • online text from the british medical journal – www.bmj.co.uk/bloodtransfusionsafety31781/o3.

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Blood transfusion

  • 1.
  • 2.
  • 3.
  • 4.
  • 5. introduction •BLOOD TRANSFUSION IS DEFINED AS THE PROCESS OF RECEIVING BLOOD PRODUCTS INTO ONE’S CIRCULATION INTRAVENOUSLY. THIS IS USUALLY DONE AS A LIFE SAVING MANEUVER TO REPLACE BLOOD CELLS OR BLOOD PRODUCTS LOST THROUGH SEVERE BLEEDING, DURING SURGERY WHEN SEVERE BLOOD LOSS OCCURS OR TO INCREASE THE BLOOD COUNT IN AN ANAEMIC PATIENT. •TRANSFUSIONS USUALLY INVOLVE THE USE OF TWO SOURCES OF BLOOD – ONE’S OWN (AUTOLOGOUS TRANSFUSION) OR SOMEONE ELSE’S (ALLOGENIC TRANSFUSION). •BLOOD TRANSFUSIONS INVOLVES THE USE OF WHOLE BLOOD , RED BLOOD CELLS, WHITE BLOOD CELLS, PLASMA, CLOTTING FACTORS AND PLATELETS.
  • 6.
  • 7. Blood and blood products •BLOOD IS COLLECTED FROM DONORS WHO HAVE BEEN PREVIOUSLY SCREENED TO EXCLUDE ANY BLOOD OR BLOOD PRODUCTS THAT MAY HAVE THE POTENTIAL TO HARM THE PATIENT. •EACH UNIT OF BLOOD IS TESTED FOR EVIDENCE OF HEPATITIS-B, HEPATITIS-C , HUMAN IMMUNODEFICIENCY VIRUS I & II AND SYPHILIS. •THE ABO AND RHESUS D BLOOD GROUP IS DETERMINED AS WELL AS THE PRESENCE OF IRREGULAR RED CELL ANTIBODIES. •THE BLOOD IS THEN PROCESSED INTO SUB-COMPONENTS.
  • 8.
  • 9. WHOLE BLOOD •WHOLE BLOOD IS UNSEPARATED BLOOD CONTAINING AN ANTICOAGULANT –PRESERVATIVE SOLUTION. ONE UNIT OF WHOLE BLOOD CONTAINS - • 450 ml OF DONOR BLOOD. • 50 ml OF ANTICOAGULANT-PRESERVATIVE SOLUTION. • HAEMOGLOBIN approx. 12g/ml & HAEMATOCRIT 35% - 45%. • NO FUNCTIONAL PLATELETS. •SINCE IT IS NOT STERILIZED, CAPABLE OF TRANSMITTING ANY AGENT PRESENT IN CELLS OR PLASMA WHICH HAS NOT BEEN DETECTED BY ROUTINE SCREENING. •HOWEVER WHOLE BLOOD TRANSFUSION HAS SIGNIFICANT ADVANTAGES OVER PACKED CELLS AS IT IS COAGULATION FACTOR RICH AND IF FRESH, MORE METABOLICALLY ACTIVE THAN STORED BLOOD.
  • 10. • STORED BETWEEN +2 AND +6 DEGREES CENTIGRATE IN A BLOOD BANK REFRIGERATOR. •TRANSFUSION SHOULD BE STARTED WITHIN 30 MINUTES OF REMOVAL FROM THE REFRIGERATOR AND COMPLETED WITHIN 4 HOURS OF COMMENCEMENT BECAUSE CHANGES IN THE COMPOSITION MAY OCCUR DUE TO RED CELL METABOLISM. INDICATIONS – •RED CELL REPLACEMENT IN ACUTE BLOOD LOSS WITH HYPOVOLAEMIA •EXCHANGE TRANSFUSION CONTRAINDICATIONS – •CHRONIC ANAEMIA •INCIPIENT CARDIAC FAILURE
  • 11.
  • 12. PACKED RED CELLS •PACKED RED CELLS ARE CELLS THAT ARE SPUN DOWN AND CONCENTRATED. •ONE UNIT OF PACKED RED CELLS IS APPROX. 330 ml AND HAS A HAEMATOCRIT OF 50-70%. •THEY ARE STORED IN A SAG-M (SALINE-ADENINE-GLUCOSE- MANNITOL) SOLUTION TO INCREASE THEIR SHELF LIFE TO 5 WEEKS AT 2-6 DEGREES CENTIGRATE. •IT CARRIES THE SAME INFECTION RISK AS IN WHOLE BLOOD. •INDICATED IN REPLACEMENT OF RED CELLS IN ANAEMIC PATIENTS AND ALSO USED WITH CRYSTALLOID AND COLLOID SOLUTIONS IN ACUTE BLOOD LOSS CONDITIONS.
  • 13.
  • 14. FRESH FROZEN PLASMA •FRESH FROZEN PLASMA IS RICH IN COAGULATION FACTORS. •IT IS SEPARATED FROM WHOLE BLOOD AND STORED AT -40 TO -50 DEGREES CENTIGRATE WITH A 2 YEAR SHELF-LIFE. •IT IS THE FIRST LINE THERAPY IN THE TREATMENT OF COAGULOPATHIC HAEMORRHAGE. •ALSO USED IN THE REPLACEMENT OF MULTIPLE COAGULATION FACTOR DEFICIENCIES LIKE LIVER DISEASE, WARFARIN OVERDOSE, DEPLETION OF COAGULATION FACTORS IN PATIENTS RECEIVING LARGE VOLUME TRANSFUSIONS, DISSEMINATED INTRAVASULAR COAGULATION AND THROMBOTIC THROMBOCYTOPENIC PURPURA.
  • 15. PRECAUTIONS – •ACUTE ALLERGIC REACTIONS ARE COMMON •SEVERE LIFE THREATENING ANAPHYLACTIC REACTIONS OCCASSIONALLY OCCUR. •DOSAGE – INITIAL DOSE OF 15ml/Kg.
  • 16. Platelets •PLATELETS ARE SUPPLIED AS A POOLED PLATELET CONCENTRATE CONTAINING ABOUT 250 X 10 9 CELLS PER LITRE. •PLATELETS ARE STORED ON A SPECIAL AGITATOR AND HAVE A SHELF LIFE OF ONLY 5 DAYS. •ARE USUALLY GIVEN TO PATIENTS WITH THROMBOCYTOPENIA OR THOSE WITH PLATELET DYSFUNCTION WHO ARE BLEEDING OR UNDERGOING SURGERY AND IN PATIENTS WITH BONE MARROW FAILURE. •NOT INDICATED IN – • PATIENTS WITH ITP, TTP, UNTREATED DIC AND IN CASES OF HYPERSPLENISM.
  • 17. •DOSAGE – 1 UNIT OF PLATELET CONCENTRATE /10 kg BODY WEIGHT. •4-6 DONOR UNITS OF PLATELET CONCENTRATES WILL RAISE THE PLATELET COUNT BY 20-40 X 109/L. INCREMENT WILL BE LESS IF THERE IS ASSOCIATED SEPTICEMIA, DIC, SPLENOMEGALY. •COMPLICATION S– FEBRILE AND ALLERGIC URTICARIAL REACTIONS ARE COMMON ESPECIALLY IN PATIENTS RECEIVING MULTIPLE TRANSFUSIONS. • PATIENTS ON ASPIRIN THERAPY RARLELY POSE A PROBLEM BUT THOSE PATIENTS ON CLOPIDOGREL WHO ARE ACTIVELY BLEEDING AND UNDERGOING MAJOR SURGERY MUST BE GIVEN A CONTINUOUS INFUSION DURING THE COURSE OF THE PROCEDURE.
  • 18.
  • 19. CRYOPRECIPITATE •CRYOPRECIPITATE IS A SUPERNATANT PRECIPITATE OF FRESH FROZEN PLASMA AND IS RICH IN FACTOR VIII AND FIBRINOGEN. •IT IS STORED AT -30 DEGREES CENTIGRATE WITH A 2 YEARS SHELF LIFE. •INDICATED IN LOW FIBRINOGEN STATES (<1g/L) OR IN CASES OF FACTOR VIII DEFICIENCY (HAEMOPHILIA-A), VON WILLEBRAND’S DISEASE AND AS A SOURCE OF FIBRINOGEN IN DISSEMINATED INTRAVASCULAR COAGULATION. •POOLED UNITS CONTAINING 3-6 gms FIBRINOGEN IN 200-500 ml RAISES THE FIBRINOGEN LEVEL BY APPROX. 1g/L. •MUST BE INFUSED WITHIN 6 HOURS.
  • 20.
  • 21. BLOOD GROUPS AND CROSS-MATCHING •HUMAN RED BLOOD CELLS HAVE MANY DIFFERENT ANTIGENS ON THEIR CELL SURFACE. •TWO GROUPS OF ANTIGENS ARE OF MAJOR IMPORTANCE IN MEDICAL PRACTICE – THE ABO AND THE RHESUS SYSTEMS. •ABO SYSTEM-THESE ARE STRONGLY ANTIGENIC AND ARE ASSOCIATED WITH NATURALLY OCCURING ANTIBODIES IN THE SERUM.THIS SYSTEM CONSISTS OF 3 ALLELIC GENES A,B & O. •GROUP A & B CONTAIN SPECIFIC ANTIGENS AND PROVOKE A REACTION IF THESE ANTIGENS ARE NOT PRESENT IN THE RECIPIENT. •GROUP ‘O’ CONTAINS NO ANTIGENS TO PROVOKE A REACTION IN THE RECIPIENT AND HENCE CALLED ‘AMORPHS’.
  • 22. •THEREFORE, BLOOD GROUP ‘O’ IS CONSIDERED AS THE UNIVERSAL DONOR AS IT HAS NO ANTIGENS TO PROVOKE A REACTION AND ‘AB’ BLOOD TYPE IS CONSIDERED AS THE UNIVERSAL RECIPIENTS AS THEY HAVE NO CIRCULATING ANTIBODIES TO THEM. •RHESUS SYSTEM- THE RHESUS D ANTIGEN IS STRONGLY ANTIGENIC AND IS PRESENT IN APPROXIMATELY 85% OF THE POPULATION. ANTIBODIES TO THE ‘D’ ANTIGEN ARE NATURALLY NOT PRESENT IN THE REMAINING 15% OF THE INDIVIDUALS BUT THEIR FORMATION MAY BE STIMULATED BY THE TRANSFUSION OF RH’+’ RED CELLS OR THEY MAY BE ACQUIRED DURING DELIVERY OF A RH-D-POSITIVE BABY LEADING TO HAEMOLYTIC DISEASE OF THE NEWBORN IN A SUBSEQUENT PREGNANCY.
  • 24. •IF USED CORRECTLY, BLOOD TRANSFUSION CAN BE LIFE-SAVING, INAPPROPRIATE USE CAN ENDANGER LIFE. •THE DECISION TO TRANSFUSE BLOOD OR BLOOD PRODUCTS SHOULD ALWAYS BE BASED ON A CAREFUL ASSESSMENT OF CLINICAL AND LABORATORY INDICATIONS THAT TRANFUSION IS NECESSARY TO SAVE LIFE OR PREVENT SIGNIFICANT MORBIDITY.
  • 25. minimising the need for blood transfusion •Preoperative planning- •History and examination including surgical or bleeding history •Full blood count, blood chemistry, coagulation, •Consider autologous blood deposit •Consider erythropoietin to boost haemoglobin concentration •Treat iron or folate deficiency •Stop aspirin prophylaxis if possible •Day of admission •Check if taking aspirin, non-steroidal anti-inflammatory drugs, anticoagulants •Repeat full blood count •Consider drugs to reduce bleeding (such as aprotinin)
  • 26. During surgery •Be prepared for longer duration to secure haemostasis •Consider hypotensive surgery if appropriate •Avoid hypothermia—give all fluids through a warmer •Consider fibrin glues and sealants Postoperative care •Accept lower postoperative haemoglobin concentration •Accept transfusions of just one unit of blood, to exceed transfusion trigger •Use continuous face mask oxygen if patient has low haemoglobin concentration •Prescribe iron and folic acid routinely •Consider Tranexamic acid
  • 27.
  • 28. •EXTERNAL BLEEDING & MEDICAL CONDITIONS LIKE THALASSEMIA. •INTERNAL BLEEDING –Eg. VARICEAL BLEEDING,ECTOPIC PREGNANCY, ANTEPARTUM HAEMORRHAGE , RUPTURED UTERUS, TRAUMATIC INJURIES TO THE CHEST, SPLEEN, PELVIS, LUNGS, RED CELL DESTRUCTION AS IN MALARIA, SEPSIS, DISSEMINATED INTRAVASCULAR COAGULATION. •CARDIORESPIRATORY STATE AND TISSUE OXYGENATION – BP, PULSE, RESPIRATORY RATE, CAPILLARY REFILL TIME, PERIPHERAL PULSES, TEMPERATURE, URINE OUTPUT, CARDIAC FAILURE. •ASSESSMENT OF ANAEMIA – CLINICALLY FROM THE TONGUE, PALMS, EYES, NAILS AND FROM LABORATORY ASSESSMENT OF THE HAEMOGLOBIN LEVEL OR HAEMATOCRIT. •ANTICIPATED SURGERY WHERE POST-OPERATIVE BLOOD LOSS IS HIGHLY PROBABLE , CONTINUOUS BLEEDING OR LIKELIHOOD OF RECURRENCE OF BLEEDING, CONTINUING HAEMOLYSIS.
  • 29. CAUSES OF ACUTE BLOOD LOSS IN AN OBSTETRIC PATIENT •FETAL LOSS IN PREGNANCY – INCOMPLETE ABORTION, SEPTIC ABORTION. •ECTOPIC PREGNANCY – TUBAL, ABDOMINAL. •ANTEPARTUM HAEMORRHAGE – PLACENTA PREVIA, ABRUPTIO PLACENTAE, RUPTURED UTERUS, VASA PRAEVIA. •TRAUMATIC LESIONS – EPISIOTOMY, PERINEAL OR CERVICAL LACERATIONS, RUPTURED UTERUS. •POST-PARTUM HAEMORRHAGE – UTERINE ATONY, RETAINED PRODUCTS OF CONCEPTION, TRAUMATIC LESIONS, PUERPERAL SEPSIS, TISSUE DAMAGE FOLLOWING OBSTRUCTED LABOUR, BREAKDOWN OF UTERINE WOUND AFTER CAESAREAN SECTION. •DISSEMINATED INTRAVASCULAR COAGULATION INDUCED BY – IUFD, AMNIOTIC FLUID EMBOLISM, PRE-ECLAMPSIA, ABRUPTIO PLACENTAE, INDUCED ABORTION, RETAINED PRODUCTS OF CONCEPTION.
  • 30. PERI-OPERATIVE RED BLOOD CELL TRANSFUSION CRITERIA HAEMOGLOBIN INDICATION LEVEL g/dl <6 Probably will benefit from transfusion 6-8 Transfusion unlikely to be of benefit in the absence of bleeding or impending surgery >8 No indication for transfusion
  • 31. Who Transfusion guidelines for chronic anaemia during pregnancy DURATION OF PREGNANCY HAEMOGLOBIN LEVEL CONSIDER IF- <36 WEEKS 5.0 g/dl or LESS EVEN Hb 5.0-7.0g/dl + Established WITHOUT CLINICAL SIGNS or incipient cardiac failure, OF CARDIAC FAILURE OR Clinical evidence of hypoxia, HYPOXIA Pneumonia or any serious bacterial infections, Pre- existing heart disease. >36 WEEKS 6.0 g/dl OR LESS Hb 6.0 – 8.0 g/dl + Above mentioned conditions ELECTIVE CAESAREAN 8.0-10.0 g/dl- Confirm blood Elective CS Planned + SECTION group, Save freshly taken History of APH, PPH, serum for cross-matching. Previous CS. <8.0 g/dl – 2 Units of blood should be cross-matched and available.
  • 32. ESTIMATING BLOOD LOSS •IN ORDER TO MAINTAIN BLOOD VOLUME ACCURATELY, IT IS ESSENTIAL TO CONTINUALLY ASSESS SURGICAL BLOOD LOSS THROUGHOUT THE PROCEDURE. BLOOD VOLUME NEONATES 85-90ml/kg Body Weight CHILDREN 80ml/kg Body Weight ADULTS 70ml/kg Body Weight Example: An adult weighing 60 kgs would have a blood volume equal to 70x60, which is 4200 ml. 1. Weigh swabs while still in their dry state. 2. Weigh the blood soaked swabs as soon as they are discarded and subtract their dry weight (1ml of blood weighs approximately 1 gm). 3. Weigh the ungraduated drains or suction bottles and subtract their empty weight.
  • 33. 4. Estimate blood loss into surgical drapes, together with that pooling beneath the patient and onto the floor. 5. Note the volume of any irrigation or wash out fluids that are used during surgery. Subtract this volume from the measured blood loss to arrive at a final estimate. • IN POST-OPERATIVE TRANSFUSION CASES, THE HAEMOGLOBIN LEVEL, URINE OUTPUT, BLOOD PRESSURE, PULSE RATE, HEART RATE, CAPILLARY REFILL TIME, COLOUR OF MUCOUS MEMBRANES, RESPIRATORY RATE AND SYMPTOMS AND SIGNS OF HYPOXIA SHOULD BE CAREFULLY MONITORED.
  • 34. WHO ACCEPTABLE BLOOD LOSS GUIDELINE METHOD HEALTHY PATIENT AVERAGE CLINICAL POOR CLINICAL CONDITION CONDITION PERCENTAGE METHOD – 30% 20% <10% Acceptable loss of blood volume HAEMODILUTION METHOD – Lowest 9g/dl or 10g/dl or 11g/dl or acceptable Haematocrit Haematocrit Haematocrit Haemoglobin or Haematocrit = 27% = 30% =33% During surgery, however the decision to transfuse will ultimately need to be based on the careful assessment of Volume of blood loss, Rate of blood loss, Patient’s clinical response to blood loss and fluid replacement therapy & signs indicating inadequate tissue oxygenation.
  • 35. SAFE BLOOD TRANSFUSION PROCEDURES
  • 36. • EVERY HOSPITAL SHOULD HAVE WRITTEN STANDARD OPERATING PROCEDURES FOR THE ADMINISTRATION OF BLOOD PRODUCTS LIKE THE ONE WE HAVE IN OUR HOSPITAL , PARTICULARLY FOR THE FINAL IDENTITY CHECK OF THE PATIENT, THE COMPATIBILITY LABEL DETERMINING THE PATIENT’S ABO AND RH-D GROUP, UNIQUE DONATION NUMBER OF THE BLOOD PACK, BLOOD GROUP OF THE BLOOD PACK, THE DATE OF COLLECTION AND THE EXPIRY DATE, THE INDICATION FOR TRANSFUSION, SIGNATURE OF THE CLINICIAN PERFORMING THE PRE-TRANSFUSION IDENTITY CHECK AND THE TRANSDUSION PROCEDURE •THE BLOOD PACK SHOULD ALWAYS BE INSPECTED FOR SIGNS OF DETERIORATION ON ARRIVAL AND BEFORE TRANSFUSION IF NOT USED IMMEDIATELY. •DISCOLOURATION OF THE BLOOD PACK AND ANY SIGNS OF LEAKAGE INDICATE CONTAMINATION AND COULD CAUSE A SEVERE FATAL REACTION IF TRANSFUSED.
  • 37. DISPOSABLE EQUIPMENT FOR BLOOD ADMINISTRATION • CANNULAS MUST BE STERILE AND MUST NEVER BE REUSED. • FLEXIBLE PLASTIC CANNULAS SHOULD BE USED AS THEY ARE SAFER AND PRESERVE THE VEINS. FOR WHOLE BLOOD, RED CELLS, PLASMA & CRYOPRECIPITATE •USE A NEW STERILE BLOOD ADMINISTRATION SET CONTAINING AN INTEGRAL 170-200 micron FILTER • CHANGE THE SET AT LEAST 12 HOURLY DURING BLOOD COMPONENT INFUSION. • IN A WARM CLIMATE, CHANGE THE SET MORE FREQUENTLY AND USUALLY AFTER EVERY 4 UNITS OF BLOOD IF GIVEN WITHIN A 12 HOUR PERIOD.
  • 38. • THERE IS NO EVIDENCE THAT WARMING BLOOD IS BENEFICIAL TO THE PATIENT WHEN INFUSION IS SLOW. AT INFUSION RATES >100ml/minute, COLD BLOOD MAY BE A CONTRIBUTING FACTOR IN CARDIAC ARREST. HOWEVER, KEEPING THE PATIENT WARM IS PROBABLY MORE IMPORTANT THAN WARMING THE INFUSED BLOOD ! • WARMED BLOOD IS MOST COMMONLY REQUIRED IN LARGE VOLUME RAPID TRANSFUSIONS & EXCHANGE TRANSFUSION IN INFANTS. •BLOOD SHOULD ONLY BE WARMED IN A BLOOD WARMER THAT HAVE A VISIBLE THERMOMETER AND AN AUDIBLE WARNING ALARM AND SHOULD BE PROPERLY MAINTAINED.
  • 39. INTRAVENOUS CANNULATIONS FOR BLOOD TRANSFUSION CAN BE DONE FROM – • CEPHALIC VEIN • BASILIC VEIN • FOREARM VEINS • GREAT SAPHENOUS VEINS
  • 40.
  • 41. MONITORING THE TRANSFUSED PATIENT 1. FOR EACH UNIT OF BLOOD TRANSFUSED, MONITOR THE PATIENT: • BEFORE STARTING THE TRANSFUSION • 15 MINUTES AFTER STARTING THE TRANSFUSION • AT LEAST EVERY HOUR DURING TRANSFUSION • ON COMPLETION OF THE TRANSFUSION • 4 HOURS AFTER COMPLETING THE TRANSFUSION 2. AT EACH OF THESE STAGES, RECORD: • PATIENT’S GENERAL APPEARANCE • BLOOD PRESSURE, PULSE, RESPIRATORY RATE • FLUID BALANCE – ORAL AND IV FLUID INTAKE & URINARY OUTPUT.
  • 42. 3. RECORD: • TIME WHEN THE TRANSFUSION IS STARTED. • TIME WHEN THE TRANSFUSION IN COMPLETED. • VOLUME AND TYPE OF ALL PRODUCTS TRANSFUSED. • BLOOD PACK NUMBERS. • ANY ADVERSE EFFECTS. SEVERE REACTIONS MOST COMMONLY PRESENT IN THE FIRST 15-30 MINUTES OF A TRANSFUSION THEREFORE THEY SHOULD BE CLOSELY MONITORED DURING THIS TIME. IF THE PATIENT APPEARS TO BE EXPERIENCING AN ADVERSE REACTION THE TRANSFUSION MUST BE IMMEDIATELY STOPPED AND URGENT MEDICAL ASSISTANCE SHOULD BE SEEKED FOR.
  • 43. REFERENCES: • the who handbook on the clinical use of blood – who blood transfusion safety , geneva , 2007. • bailey & love’s short practice of surgery – 25th edition – 2008. • davidson’s principle & practice of medicine – 21st edition – 2010. • essential paediatrics – o.p. ghai – 6th edition. • online text from the british medical journal – www.bmj.co.uk/bloodtransfusionsafety31781/o3.