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Dr Salwa Hindawi

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Blood Transfusion In Neonates and Children Dr Salwa Hindawi MSc, FRCPath, CTM Medical Director of Blood Transfusion Services KAUH, Jeddah Makah 28th April2008 – PowerPoint PPT presentation

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Title: Dr Salwa Hindawi


1
Blood Transfusion In Neonates and Children
  • Dr Salwa Hindawi
  • MSc, FRCPath, CTM
  • Medical Director of Blood Transfusion Services
  • KAUH, Jeddah


  • Makah 28th
    April2008

2
Introduction
  • Blood Transfusion is not without hazards
  • you should weigh the risk against benefit
  • use of right products to the right patient at
    the right time

3
Consider
1. Child will live long enough to get a long term
complication of blood transfusion 2. children
has special need 3.Lack of evidence for many
transfusion practice in children ,depending on
adult experience and clinical judgment.
4
  • use of clinical guidelines may provide the
    following
  • improvements in outcomes.
  • improvements in medical practice.
  • decision support tools for practitioners.
  • points of reference for medical orientation and
  • education.
  • criteria for self-evaluation.

5
Pretransfusion testing in Infants less than 4
month of age
  • Maternal sample
  • ABO RhD group Antibody screen.
  • Infant samples
  • ABO RhD group Direct antiglobulin test (DAT).
  • Antibody screen (if maternal sample unavailable).
  • If no atypical Antibody in maternal infant
    serum DAT on infant red cell is negative, Cross
    matching is unnecessary.
  • After 4 month Compatibility testing is required
    as for adults.

6
cross matching within 1st 4 month of age
  • Compatibility testing is required only under the
    following conditions
  • 1. unexpected antibody is detected in the
    infant's or mother's serum
  • 2. the infant has a positive direct antiglobulin
    test result or
  • 3. the infant is to receive RBC transfusion
    incompatible with the mother's serum

7
  • For infants with ABO hemolytic disease of the
    newborn, only group O RBCs should be transfused
    until compatibility tests are nonreactive with
    ABO-specific units.
  • For plasma and platelet transfusions, infants
    should receive ABO-specific components whenever
    possible, to avoid transfusing plasma antibody
    incompatible with the infant's red cell antigens.

8
strategies to reduce donor exposure orRBC
transfusions
  • delayed clamping of the umbilical cord
  • restricting blood sampling
  • using recombinant human erythropoietin to
    stimulate erythropoiesis
  • using iron supplementation or vitamins to
    minimize the severity of anemia

9
  • using appropriately collected and stored
    multipack RBC units
  • using appropriately screened and handled RBCs
    from regular or designated donors and
  • collecting and transfusing umbilical cord blood
    (autologous blood transfusion).

10
PRBCs Specification
  • RBCs administered should be as fresh as possible
  • group O, or group specific
  • hemoglobin S negative
  • CMV-seronegative or leukoreduced
  • irradiated as indicated.

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ABO Selection of Blood Components
20
Administration of blood components
  • Pretransfusion
  • Recipient identification The name and
    identification number on the patients
    identification band must be identical with the
    name and number attached to the unit.
  • Unit identification The unit identification
    number on the blood container, the transfusion
    form, and the tag attached to the unit (if not
    the same as the latter) must agree.

21
Component Volumes to be Transfused to Children
and Neonates
  • Red cell concentrates for exchange
  • transfusion
  • Term Infant
    80-160mls/kg
  • Preterm Infant
    100-200mls/kg
  • For top-up transfusion
    10-20mls/kg
  • Platelet concentrates
  • Children weighing less than 15kg
    10-20mls/kg
  • Children weighing more than15kg
    single Apheresis unit
  • Fresh Frozen Plasma
    10-20mls/kg
  • Cryoprecipitate
    5-10mls/kg

22
Infusion flow rates RBC 3-5
mL/kg/hour FFP within 30 minutes, provided the
volume does not exceed 5-10 mL/kg Platelets
within 30 minutes. It is seldom necessary to
reduce the volume of the platelet concentrate if
the dose does not exceed 5-10 mL/kg
23
Special Products
  • Despite general measures to ensure transfusion
    safety, there still an added risk to infants and
    children with underlying hematological, oncologic
    and immunologic disorders.
  • Transfusion reaction may be caused by both
    infectious or non infectious processes.
  • Special products are blood components collected,
    processed, and selected specifically to minimize
    these complications.

24
Leucocytes Reduced Blood Components
  • Leucocytes in the blood components can lead to
    many complications
  • Universal Leucodepletion verses specific
    indications.

25
Leucodepletion of Blood Components
All neonates and intrautrine transfusion Prevent
ion of Alloimmunization in patients with AML
receiving induction chemotherapy. In patients
with other types of leukemia and in other cancer
patients receiving chemotherapy. Prevention of
Febrile Non Haemolytic Transfusion
Reaction. Replacement of CMV negative blood
components. .
26
CMV negative blood products Blood products
tested for antibodies to CMV or
leukodepleted Indicated to prevent CMV
transmission in select populations 1-Immunodefic
ient or immunosuppressed patients 2-Neonates 3-Pat
ients w/ hematologic malignancies CMV resides in
WBCs (leukodepletion), so screening not necessary
for FFP, cryoprecipitate, other plasma products.
27
4-In Oncology/BMT patients, CMV titers are
checked If patient is CMV positive, then products
do not have to be CMV negative regardless of
immune status. If patient is CMV negative, he
should receive CMV negative products
28
  • Irradiation
  • -Performed for prevention of transfusion-related
  • Graft-versus-Host Disease (GVHD)
  • -Irradiation prevents T-cells proliferation
  • 25 Gy to blood products effective
  • Used for cellular products PRBCs, platelets

29
Indications
  • premature infants lt 1200g birthweight
  • 2. infants with known or suspected congenital
  • immunodeficiency syndromes
  • 3. infants receiving granulocyte transfusions
  • 4. infants receiving directed donor blood
    component from blood relatives
  • 5. infants receiving HLA-matched or platelet
  • crossmatch-compatible platelets

30
6. infants undergoing stem cell transplants (the
stem cell product itself must not be
irradiated) 7. infants undergoing
immunosuppressive therapy, chemotherapy or
radiotherapy 8. infants receiving exchange
transfusions 9. foetuses receiving intrauterine
transfusions 10. infants receiving large volumes
of RBCs in association with ECMO.
31
Components negative for Sickle Hemoglobin
  • Sickle cell trait
  • Hb A 60
  • Hb S 40
  • Hypoxia and acidosis can lead to sickle crisis.
  • Can donate blood.

32
AABB Recommendations
  • Define patients populations who should receive
    red blood cells known to lack hemoglobin S.
  • 1- infants with small blood volume or massive
    transfusion in neonates.
  • 2- Sickle cell patients

33
Conclusions
  • Policies, Procedures and Guidelines for Blood
    Transfusion in Pediatric age group should be in
    place and implemented.
  • Training and Education for the hospital staff in
    policies, and guidelines in pediatric age group
    are important issues to be considered.
  • The use of special products is a must for
    specific patients in pediatric age group to
    ensure safety.

34
References
  • Guidelines for Transfusion Therapy of Infants
    from Birth to Four Months of age, New York State
    Council on Human Blood and Transfusion Services,
    Second Edition 2004.
  • Pediatric Transfusion, A Physicians handbook
  • 2nd Edition, 2006.
  • Prenatal and childhood transfusion, Practical
    Transfusion Medicine 2001.

35
THANKS
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