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Platelet Alloimmunization

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Why is this a big deal? ... Non-immune: Sepsis, DIC, drugs, splenomegaly, etc. Pathophysiology. WBC. HLA I ... BIG PROBLEM: Donor pool around 10,000. Of note: ... – PowerPoint PPT presentation

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Title: Platelet Alloimmunization


1
Platelet Alloimmunization
  • Joshua Field
  • June 23, 2005

2
Case
  • 24 year-old woman G0P0 with a history of AML with
    normal cytogenetics, day 20 of 73.
  • She initially presented with pancytopenia,
    including a platelet count of 6,000.
  • Prior to the initiation of her induction
    chemotherapy, she received her first platelet
    transfusion. Her platelet increment was 18,000.
  • Throughout her induction, she has received
    CMV-negative, leukoreduced, irradiated blood
    products. Platelets are single donor.

3
Case
  • On day 20, she is to receive platelet
    transfusion 9.
  • Now her platelet increment at 24 hours is 2,000.
  • Transfused another unit of single donor platelets
    and checked a 1-hour increment 3,000.
  • What to do?

4
Definition
  • Platelet refractoriness Inappropriately low
    increment in platelet count following a
    transfusion.
  • Platelet alloimmunization Formation of
    antibodies directed to foreign antigens on the
    surface of platelets.
  • Formula to determine platelet response
  • 1 hour Increment lt 5,000-7,500.
  • Corrected Count Increment
  • (Platelet increment X BSA)/Platelet dose
  • Expected gt 7500 at 10-60 minutes or gt4500 at
    18-24 hours.
  • Less than predicted platelet increment on 2
    occasions
  • Fresh platelets lt 72 hours.
  • ABO compatible.

5
Why is this a big deal?
  • Blood Rev, 1998 pp. 234-8 Recommend platelet
    transfusion threshold of 10X10(9). Blanket
    recommendation.
  • NEJM, 1997 pp. 1870-5 Newly diagnosed AML.
    Compared threshold of 10K vs. 20K. Found a
    similar bleeding risk.

6
Pathophysiology
Ibalpha
IbB
IX
IIIa
V
IIb
Ia
Platelet
ABH
IIa
CD109
B2 microglobulin
HLA I
7
Pathophysiology
  • Immune
  • HLA class I A,B. Primary trigger WBCs in
    platelet and RBC transfusions.
  • Human platelet antigens Minor role.
  • ABH
  • Blood, 1979 HLA-matched platelets with
    incompatible ABO resulted in 23 lower increment.
  • Enormous variability in expression of ABO on
    platelets.
  • Non-immune Sepsis, DIC, drugs, splenomegaly,
    etc.

8
Pathophysiology
Transfused Blood product
WBC
Anti-HLA antibodies
HLA I
Transfused Platelet
9
Prevalence and Incidence
  • Kiefel, et al, Transfusion, 2001 766-70.
  • 252 patients with solid tumor and hematological
    malignancies, heavily transfused, platelet
    refractory.
  • 42 anti-HLA antibodies.
  • 8 anti-HPA antibodies.
  • TRAP trial 27 developed LCT antibodies.

10
Risk
  • High number of transfusions?
  • Dutcher, et al, Blood, 1981 1007-11.
  • 114 patients, no transfusion history.
  • Received random donor platelets.
  • Lymphocytotoxic HLA antibody screen.
  • 42 developed a positive screen at 8 weeks.
  • About 10 at one week.
  • Antibody lost in 20.
  • Suggests early event.

11
Risk
  • Patients received pooled platelets.
  • Exposed lt20 donors 22 LCT antibody-positive.
  • Exposed 20-60 41 LCT antibody-positive.
  • Same conclusion with single donor platelets?

12
Risk
  • Does disease matter?
  • Hematological malignancies Blood, 1987 pp.
    1727-9 incidence of LCT in AML 44 vs. ALL 18.
    Contribution of steroids?
  • Blood, 1981 pp. 122-8 Heavily transfused
    patients, examine for LCT.
  • Acute leukemia 20/65.
  • Lymphoma 5/19.
  • Sarcoma 2/16.
  • Aplastic anemia 7/8.

13
Platelet refractoriness
What is etiology?
Check 1 hour and 24 hour increment
Fever, sepsis, splenomegaly, drugs, etc.
Poor increment
ABO compatible platelets
Poor increment
LAT
Positive
HLA matched/mismatched platelets/antigen negative
Poor increment
Check platelet-specific antibodies
IVIG or pray or quit transfusing platelets
14
Diagnosis and Management
  • Lymphocytotoxic antibodies
  • Patient serum and complement added to lymphocytes
    with known human leukocyte antigens.
  • Antibodies attach to HLA, activate complement,
    lyse cells.
  • Dye is added, which colors the wells of lysed
    cells.
  • Reported as a percentage reactive (what is a
    positive result?)
  • May be able to determine the target antigen.

15
Diagnosis and Management
  • American Journal of Hematology, 1983 363-70
    Screened heavily transfused patients for LCT,
    then measured platelet response.
  • Sensitivity 63.
  • Specificity 94.

16
Diagnosis and Management
  • Alloimmunized patient
  • HLA-matched platelets
  • Mismatched platelets (CREGS)
  • Antigen-negative platelets
  • HPA-negative platelets
  • Platelet crossmatch (not at Barnes)
  • IVIG

17
Diagnosis and Management
  • HLA-matched platelets
  • BJH, 1987 115-21 90 refractory patients may
    benefit.
  • American Journal of Hematology, 1977 219-26 60
    refractory patients benefit.
  • BIG PROBLEM Donor pool around 10,000.
  • Of note Barnes donor pool is about 1500. Huh?

18
Diagnosis and Management
  • Public epitope versus private epitope

HLA-A1
HLA-A3
HLA-A10
19
Diagnosis and Management
  • American Journal of Hematology, 1977 pp. 219-26.
  • Cross-reactive groups (CREGS)
  • Platelets mismatched at 1 or 2 cross-reactive HLA
    antigens produced increments similar to perfect
    matches.
  • Provides 10 times as many prospective donors.

20
(No Transcript)
21
Diagnosis and Management
  • HLA-B12 Found in 25 of population.
  • Szatkowski, et al. Tissue Antigens 1980 361-8
    HLA-B12 positive patients may have 35-fold
    differences in expression of the antigen between
    platelets.
  • Schiffer, et al. Blood 1989 1172-6 Selectively
    mismatched at B12 69 transfusion were
    successful.

22
Diagnosis and Management
  • HLA antigen negative platelets
  • If identify specificity of anti-HLA antibody
  • Antigen-negative platelets.

23
Diagnosis and Management
  • Platelet crossmatch Transfusion, 1990 314-7.
  • Perform an ELISA with stored platelets and
    patients serum.
  • 14/34 transfusions into heavily alloimmunized
    patients produced CCI gt 7500.

24
Diagnosis and Management
  • Alloimmunization to Platelet-Specific Antigens
    Not common.
  • Blood, 85 (7), 1995 pp 1736-41
  • 229 heavily transfused patients.
  • 5 patients with anti-HPA antibodies.
  • European Journal of Hematology, 56(4) 248-51
  • Anti-HPA 9.6.

25
Diagnosis and Management
  • IVIG
  • Blood, 1990 313-16 400 mg/kg for 5 days.
    Incompatible platelet donor before and after
    treatment. Improved 1-6 hour, not 24 hour.
  • American Journal of Hematology, 1991 15-23 Post
    transfusion increment increased. Best in
    patients with PRAlt85.

26
Prevention of alloimmunization
  • TRAP Study Group NEJM, 1997 1861-9
  • 530 newly diagnosed AML, no alloantibodies,
    undergoing induction chemotherapy.
  • Received
  • Random donor platelets.
  • Filtered, random donor platelets.
  • UVB, random donor platelets.
  • Filtered, single donor platelets.
  • all received filtered, leukoreduced RBCs.

27
Prevention of alloimmunization
  • Results LCT positive and refractory.
  • Random donor platelets 13
  • Filtered, random donor platelets 3
  • UVB, random donor platelets 5
  • Filtered, single donor platelets 4
  • all received filtered, leukoreduced RBCs.
  • Concluded leukoreduced, UVB beneficial. Single
    donor platelets not helpful.

28
Case
  • Transfused ABO compatible platelets 1 hour
    increment 4,000 24 hour increment 2,000.
  • Lymphocytotoxic antibody screen was performed
    PRA 90.
  • HLA-matched platelets 1 hour increment 5,000
    24 hour increment 3,000.
  • She received 2 more HLA-matched platelet
    transfusions with poor increment.

29
Case
  • Transfuse as needed for bleeding.
  • Random donor platelets anyone?
  • She has no siblings and will undergo
    consolidation chemotherapy with high-dose
    cytosine arabinoside.
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