Blood transfusion

Question 1

What is the probalem with givign RhD+ve blood to an RhD -ve patient?

Answer 1

Sensitisation –> once it is okay, but can cause formation of anti-D

–> problematic in pregnancy or future transfusion

Question 2

When is an antibody screen in blood groups done?

how and why?

Answer 2

1-3% of people have additional antibodies (outside RBO) (risk factor: several previouy transfusion )

Therefore:
IAT: INDIRECT ANTIGLOBULIN TECHNIQUE

Done before every transfusion –> (Screen: S of G&S)

IAT: bridges red cells coated by IgG, which can’t themselves bridge 2 red cells – to form a visible clump. Takes 30 mins’ incubation at 37°C

Question 3

What is an electronical crossmatch?

When can that be done?

Answer 3

Based on data on blood products and antibody testing, plasma are never physically cross -matched

Can be done with recipient who do not have any antbodies on antibody screen
–> once positive: serological crossmatch needs to be done

Question 4

How and when are serological crossmatches done?

Answer 4

Usually done if any antibodies positive – >
incubation of donor + recipeint blood for 30-40 minutes

Question 5

What are the main pillars of Patient Blood Management?

Answer 5

Generally used to optimise blood and how it can be managed

Question 6

What are the indications for transfusion or RBC?

How is it usually transfused (time and dose)

Answer 6

Before: Treat Iron/Folate/B12 deficiency first unless active bleeding

Thresholds

• Most guidelines suggest a threshold of 70g/l if asymptomatic; 80g/l if symptomatic (post-chemo: >80)
• Higher threshold of up to 90-100g/l for patients with coronary heart disease

Others

• Blood Loss: >30% of total blood

How

• Only transfuse one unit at a time unless active bleeding
• Can be transfused “stat” but routinely would be 2-3 hours

Question 7

What Red cells can be given to what blood groups ?

How are they stored and how should they be given?

Answer 7

Give ABO/D compatible
Group O (negative) in emergency

Stored at 4°C for 35 days

Must be transfused within 4 hours of leaving fridge

Transfuse 1 unit RBC over 2-3 hours

Question 8

Does ABO and D compatability need to be considered with platelet transfusion?

How are platelet transfusion stored and given?

Answer 8

ABO/D antigens weakly expressed –> **must be ABO matched **

Should be Rhesus D compatible

**Stored at 20°C for 7 days (higher risk of infection) **

Transfuse 1 unit of platelets over 20-30 minutes

Question 9

What are the indications for Platelet transfusions?

Answer 9

1. Any active bleeding / consumption (TTP, DIC, HIT)
2. Consumptive disorders e.g. TTP, DIC, HIT
   * Do not transfuse unless actively bleeding (plts will be destroyed and transfusion is ineffective)
3. If massive RBC transfusion (>75 consider transfusion to balance platelets))
4. Reduced production e.g. leukaemias
   * Transfuse when under 10bn/litre

Higher threshold of 20 in sepsis
* Pre-procedure: Various thresholds depending on procedure

5. Prevent Bleeding in surgery
   * under 50 (can be higher on vary on site (highest thresholds for eye / brain)

Question 10

What are the components of FFP?

Answer 10

Plasma, including** all coagulation factors** and plasma proteins

All cellular components are removed from the transfusion product

Unit volume: ∼200–300 mL

Question 11

What ABO / D compatibiltiy must be considered when giving Cryoprecipitate or FFP?
Why?

Answer 11

RBO must be matched (plasma will/ might still contain antibodies)

D is not important –> does not contain Red cells, therefore sensitisation is extremely rare

Question 12

What are the indications of giving FFP?

How is it stored and how is it given?

Answer 12

Coinsider using Vitamin K first if appropriate
–> Given for clotting (Pt and APTT abnormalities)

• Do not use unless patient is bleeding or undergoing a procedure e.g. surgery
• Dose depends on patient weight, INR and target INR
• Needs 30 minutes to thaw out first (stored at -24-35 °C for 24-36 months

Question 13

What are the components of Cryoprecipitate

Answer 13

Has higher Fibrinogen than FFP –>

Clotting factors (fibrinogen, factor VIII, factor XIII), vWF, and fibronectin

Question 14

What are the indications for giving cryoprecipitate?

Answer 14

• Bleeding associated with fibrinogen deficiency (e.g., due to DIC, liver disease): typically performed if serum fibrinogen is < 100–150 mg/dL
• Alternative therapy for deficiencies in clotting factors, including vWF, factor VIII, and factor XIII

Question 15

What are the indications for administration of CMV negative blood?

Why?

Answer 15

only required for intra-uterine /neonatal transfusions and

–> for elective transfusion in pregnant women (baby in-utero is exposed to maternal transfusion)

Question 16

What are the indications for administration of irradiated blood?

Answer 16

Irradiation: kills of more potential infections + donor lymphocytes

Required for highly immunosuppressed patients, who cannot destroy incoming donor lymphocytes: which can cause (fatal) transfusion associated graft versus host disease (TA-GvHD)

Question 17

What are the indicatins of administration of Washed platelts?

Answer 17

red cells and platelets are only given to patients who have severe allergic reactions to some donors’ plasma proteins (makes extra-sure that less donor’s plasma proteins are there)

But adds 4-5h to transfusion

Question 18

How can adverse reactions to blood transfusions be classified?

Answer 18

Acute under 24h
Delayed >24h

Question 19

What are the acute adverse transfusion reactions that occur <24h post-transfusion?

Answer 19

• Acute haemolytic (ABO incompatible)
• Allergic/anaphylaxis
• Infection (bacterial)
• Febrile non-haemolytic
• Respiratory - mainly 2:
  1. Transfusion associated circulatory overload (TACO)
  2. Acute lung injury (TRALI)

Question 20

What are the delayed adverse transfusion reactions that occur >24h post-transfusion?

Answer 20

• Delayed haemolytic transfusion reaction (antibodies)
• Infection : viral, malaria, vCJD (all very rare)
• TA-GvHD
• Post transfusion purpura
• Iron overload

Question 21

What are early signs of an acute transfusion reaction?

How are they monitoried

Answer 21

Can be many signs, incl. rise in temp and pulse
fall in BP
–> monitoring done via obs after first 15 min
–> hourly after until transfusion is finished

Question 22

What is the most common acute adverse reaction to a transfusion?
How is it detected?

Answer 22

Most common: Febrile non-haemolytic transfusion reaction (1 in 900 transfusions)

Rise in temperature of ≤1°C without circulatory collapse

• Caused by release of cytokines by leukocytes in donor plasma due to storage (cytokines leak)

Management

• Stop or slow-down transfusion
• may need to treat with
  paracetamol
• Prevention: use of leukodepleted blood products

Question 23

What are the clinical symptos and signs of allergic reaction to blood products?

What should be done?

Answer 23

Symptoms of anaphylaxis –> IgE mediated transfusion reaction (1 in 30.000)

Symptoms occur within minutes

• Risk increases in patients with IgA deficiency (as most commonly donor IgA is allergen –> consider IgA negative blood for patietns with IgA deficiency)

Management
1. Stop transfusion
2. Anaphylaxis protocol

Question 24

What are the clinical symptoms and signs of an ABO mismatch to blood products?

What should be done?

Answer 24

Due to ABO or other mismatch (incidence 1 in 200.00 most commonly due to sampling error)

Rapid onset during transfusion or up to 24h after transfusion IgM-mediated reaction

• Shock: fever chilld, hypotension, tachycardia
• Haemolysis: jaundice, dyspnoea, chest pain
• Can progress to: DIC, Shock, Renal failure

Question 25

What are the two respiratory acute adverse reactions to blood products?

Which one is the most common and what are the signs + symptoms?

Answer 25

TACO more common - transfusion associated circulatory overoad –> essentially presents as fluid overload and pulmonary oedema

• wihtin 6 hours of infusion
• Resp disress
• Differentiating feautre: TACO presents in patients with pre-existing heart failure /oedema (and symptoms: e.g. increased JVP)

(if at high risk –> think about diuretic administration pre-transfusion)

The other is TRALI- Transfusion-related acute lung injury

• Similar symptoms to TACO
• Abscence of heart failure –> non-cardiogenic pulmonary oedema (immune-mediated)

Question 26

How does bacterial contamination of blood products present as an acute adverse reaction to blood products?

Answer 26

Symptoms occur within minutes to hours

• More commonly occurs with platelet transfusion
• due to production of endotoxins –> can lead to quick collapse

Question 27

What is TRALI?

Answer 27

Transfusion-related acute lung injury

Symptoms similar to TACO

• Caused by interaction with anti-HLA antibodies in donor blood with recipient
• Transfusion-related acute lung injury
• Abscence of heart failure –> non-cardiogenic pulmonary oedema (immune-mediated)

Question 28

What is delayed haeolytic transfusion reaction?
Explain the pathophysiology

Answer 28

Occurs within 1 week of transfusion in 1 in 22.000 transfusions

IgG mediated response to foreign blood products –> usually in patients who have recieved previous transfusions and have formed allo-antibodies against minor blood proteins –> binding of alloantibodies to donor RBCs causing extravascular hemolysis

Presentation:
* often asymptomatic
* otherwise: mild symptoms (fever, jaundice, anaemia, chest, abdomen or back pain)

Question 29

How does Delayed Haemolitc transfusion reaction present?
how do you test for it?

Answer 29

Haemolysis screen

• Bilirubin
• LDH
• Retics
• Hb
• DAT (positive)
• Haemoglobinuria over few days
  Test U&Es – as can cause renal failure
  Repeat G&S for ? new antibody

Question 30

What is Transfusion Associated Graft versos host disease?
What is the pathophysiology?
How do you prevent it?

Answer 30

Rare reaction to blood transfusion

Normally: donors blood lymphocytes are destroyed, but in very immunosuppressed patients: donor lymphocytes are not destroyed
–> Lymphocyte-mediated graft vs. host disease

Prevention: use irradiated blood products in very immunosuppressed patients (depleted
lymphocytes)

Presentation: Symptoms include diarrhoea, liver failure, skin desquamation and bone marrow failure

But: always fatal

Question 31

What tis post-transfusion purpura?
How common is it, how is it treated?

Answer 31

• Relatively rare transfusion reaction
• Due to previous sensitisation to platelt antigens –> mainly in women with multiple pregnancies or multiple blood transfusions

–> Antibody formation against donor platelets (+ destructions of own platelts, unknown why)

Appears 7-10 days post transfusion
* usually resolves in 1-4 weeks, but can cause significant bleeding

Management
* IvIG
*

Question 32

What is Haemolytic disease of the Newborn?

Answer 32

IgG antibodies against Rhesus factor (from a rh- mother sensitised to D carrying a Rh+ve baby)

–> crossing of IgG antibdoies over placenta
–> destruction of fetal blood
–> presents as
* foetal anaemia
* Haemolytic disease of newborn (anaemia plus high bilirubin - which builds up after birth as no longer removed by placenta)

Question 33

What are the clinical features of haemolytic disease of the newborn?

Answer 33

• Neonatal anemia
• Hepatosplenomegaly
• Neonatal jaundice
• Usually present at birth or manifests within the first 24 hours of life
• In Rh incompatibility, unconjugated bilirubin levels may be dangerously high, causing kernicterus.
• Hypoxia
• Prematurity
• Scattered petechiae (rare but associated with poor prognosis)

Question 34

How would you manage pregnancies if mother already has anti-d antibodies formed?

Answer 34

• Monitor fetus for anaemia – MCA Doppler ultrasound
• Deliver baby early, as HDN gets a lot worse in last few weeks of pregnancy
• If severe: intrauterine blood transfusions

Question 35

How does anti-D to prevent maternal blood sensitisation given in pregnancy work?

Answer 35

RhD positive (fetal) red cells get coated with anti-D Ig and then they get removed by the mother’s reticulo-endothelial system (spleen) before they can sensitise the mother to produce anti-D antibodies