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    Lab BB 10

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    Lab BB 10

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    2010035
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    LAB BB 10

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    Lab BB 10

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    of 20

    ANTIBODY SCREENING

    Dr. salim alawneh


    Lab 10
    Antibody Screening

    Antibody Detection and Identification

    Purpose
     The purpose of the antibody screen is to detect red blood cell
    antibodies other than anti-A or anti-B.
     These antibodies are called “unexpected” because only
    0.3 to 2 % of the general population have positive
    antibody screen.
     Once an unexpected antibody is detected, antibody
    identification studies are performed to determine the
    antibodies specificity and clinical significance.
    Antibody Screening

    All red blood cell antibodies are significance if they cause


    shortened survival of antigen positive red blood cells. For
    example, anti-D is a clinically significant antibody,
    because it will bind to D-positive red blood cells,
    resulting in immune destruction or hemolysis.

    Proper detection and identification of red blood cell


    antibodies is important for the selection of appropriate
    blood for transfusion and in the investigation of
    hemolytic disease of the new born, and immune
    hemolytic anemia.
    Antibody Screening

     Antibody screening test involve testing patient’s serum


    against two or three reagent red blood cell samples called
    screening cells

     Screening cells are commercially prepared group O cell


    suspensions obtained from individual donors that are
    phenotype for the most commonly encountered and
    clinically important red blood cell antigens.
    Antibody Screening

     Group O cells are used so that naturally occurring anti-A


    or anti-B will not interfere with detection of unexpected
    antibodies.

     The cells are selected so that the following antigens are


    present on at least one of the cell sample;
    D, C, E, c, e, M N, S, s, P, Lea, Leb, K, k, Fya, Fyb, and Jkb.
    Antibody Screening

     An anti-gram listing the antigen makeup of each cell


    provided with each lot of screening cells issued from a
    manufacture. It is important that the lot number on the
    screening cells matches the lot number printed-On the
    anti-gram because antigen make up will vary with each lot.

     The “ideal” screening cells have red cells with homozygous


    expression of as many antigens as possible.
    Antibody Screening

     There is no requirement that screening cells contain red


    cells with homozygous expression of antigens, however,
    the most workers prefer that such red cells are included
    in screening cells sets because many antibodies,
    especially JK and M antibodies, show dosage effect and
    give stronger reactions when tested against cells with
    homozygous expression of their corresponding antigen.
    Antibody Screening

     As a result of dosage, weakly reacting antibody may not


    be detected if serum samples are not tested against red
    cells with homozygous expression of the their
    corresponding antigen.
    Antibody Screening

    Screening Cells.
     The screening cells are available in three form
    1- a single vial of no more than two donors pooled
    together in one vial.
    2- two vials each with a different donor.
    3- 3 vials representing three different donors.

    Two or three cells screening sets are required for


    detection of antibodies in pre-transfusion testing.
    Antibody Screening

    Detection of very low levels of antibody in a


    recipient’s serum is important because
    transfusion of antigen-positive red cells may
    result in a secondary immune response with
    rapid production of antibody and subsequent
    destruction of transfused red blood cells.
    Antibody Screening

    Red blood cells should be re-suspended by gentle


    shaking or tilting the tube until the cells no longer adhere
    to the sides. Agglutination is graded once the red blood
    cells are re-suspended.

    Agglutination reactions are routinely graded as negative


    (no agglutination).

    Weakly positive, and 1+ through 4+. The degree of the


    positive reaction generally indicates the amount of Ab
    present not its significance.
    Antibody Screening

    Auto-logous Control.
     Autologous control is considered as part of the Ab
    screening, it can be performed in parallel with the Ab
    screen and involves testing the patient’s serum against
    the patient’s red blood cells.

     A positive auto-logous control is an abnormal finding


    and usually means that patient has a positive direct
    antiglobulin test (DAT).
    Antibody Screening

    Grading Reactions.
     Aggregation or hemolysis of test red blood cells is the
    visible end point of an Ab-Ag interaction.

     Test results should be read immediately after


    centrifugation as delays in reading may cause elution of
    antibody and false- negative test results

     The first step in reading hem-agglutination reactions is


    inspection of the supernatant for signs of hemolysis (red
    or pink coloration).
    Antibody Screening

    Interpretation.
    Evaluation of the antibody screening and auto-
    logous control results can provide clues and give
    direction for the identification and resolution of
    the Ab or Abs. The investigator should consider
    the following questions;
    Interpretation

     1- In what phase (s) did the reaction (s) occur?

     Low temperature: Abs of the IgM class will react best at


    low temperatures and are capable of causing
    agglutination of saline-suspended red blood cells
    (immediate spin reading (IS). Of the commonly
    encountered Abs are, anti-N, -I. and -P (IgM)

     Abs of the IgG class will react best at the AHG Phase
    (37°C). Of the commonly encountered Abs are; anti-Rh,
    kell, Kidd, and Duffy (IgG).

     Where as Lewis, M, Abs may be IgG, IgM, or a mixture of


    both.
    Interpretation

     2- Is the auto-logous control negative or positive?

     A positive Ab screen and a negative auto-logous control indicate an


    allo-antibodv has been detected.

     A positive auto-logus control may indicate the presence of auto-


    antibodies, antibody to medication or it may idiopathic

     If the patient has been recently transfused, the positive


    auto-logous control may be due to alloantibody coating
    circulating donor red blood cells.
    Interpretation

     3- Did more than one screening cell react and if so, did
    they react at the same strength and phases?

     If the patient has multiple Abs, when the Abs


    corresponding Ag is found on more than one screening
    cell, or when the patient’s serum contains an
    autoantibody, more than one screening cell will be
    positive.
     A single Ab specificity should be suspected when all cells
    react at the same phase and strength.
     Multiple Abs are most likely when cells react at different
    phases and strengths and auto-antibodies are suspected
    when the auto-logous control is positive.
    Interpretation

     4-Are the cells truly agglutinated or rouleaux present?

     Serum from patients with multiple myeloma or who have


    received high molecular weight plasma expanders
    (dextran) may cause non-specific aggregation of red
    blood cells known as rouleaux.

     Rouleaux is not a significant finding in Ab screening


    tests but it is easily confused with Ab mediated
    agglutination. To differentiate between rouleaux and
    agglutination;
    Interpretation

     1- Rouleaux cells have “a stacked coin” appearance when


    viewed microscopically.

     2- It will not interfere with the AHG phase of testing


    because the patient’s serum is washed away prior to the
    addition of the AHG reagent.

     3- It is observed in Ab tests containing the patient’s


    serum including the auto-logous control and the reverse
    ABO typing.
     4- Rouleaux is dispersed by the addition of 1 to 3 drops of
    saline to the test tube.
    Reagent Red Blood Cell Screening Cell
    Sectional Listing of Antigens Present

    F F J J L
    L P I 3
    D C E c e K k y y k k e S s M N AHG CC
    No a b a b ea b 1 S 7
    cell
    I + + 0 ++ + 0 0 + + + 0 + + + + 0 + 0 0 2+

    II + 0 + +0 0 + + 0 + 0 0 + 0 + + 0 + 0 0 0 2+

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