Transfusion management for patients taking an anti-CD38 monoclonal antibody

Bub, Carolina Bonet; Reis, Isabel Nagle; Aravechia, Maria Giselda; Santos, Leandro Dinalli; Bastos, Eduardo Peres; Kutner, José Mauro; Castilho, Lilian

doi:10.1016/j.bjhh.2017.09.003

Cited by 13 publications

(22 citation statements)

References 16 publications

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“…Phenotyping may be inaccurate if a patient has received a blood transfusion in the previous 3 months [39,40]. In this case, the genotype is unaff ected, and blood group genotyping is the method of choice [22,41,42].…”

Section: The Topic Position In Scientific/professional Publicmentioning

confidence: 99%

The role of the Kidd-antibodies in posttransfusion reactions

Nikolić¹,

Čolak²,

Kadija³

et al. 2019

Hosp Pharm Int Multi J

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Topic: The Kidd blood group (Jk) was discovered in 1951 and according to International Society for blood transfusion (ISBT) the Kidd (Jk) blood group is registered under the number 009. Antigens of the Kidd system are detected only on RBCs and kidney. Incompatibile transfusion in Jk blood group can provoke sensitization and appearance of anti-Jka or anti-Jkb antibodies. Jk antibodies are common cause of delayed hemolytic transfusion reactions (DHTRs). Although Kidd antibodies can lead to acute reactions, kidney damage and hemoglobinuria are very rare. More important is Kidd-antibody ability for delayed hemolytic reactions. The aim is to underline Jka antibodies laboratory characteristics, their role in delayed posttransfusion reactions and possible complications of blood transfusions. The topic position in scientifi c/professional public: Kidd-antibodies, usually, destroy transfused red cells after a variable period of between 7 and 21 days. DHTR is the result of anti-Jka antibodies tendency to fall rapidly to undetectable levels even after incompatible transfusion. Anti-Jka has been reported as reason for kidney transplant rejection. There were examples of anti-Jka that react only when preservatives such as p-hydroxybenzoic acid (parabens), Na-azide or related compounds, antibiotics are present in the reaction mixture. Also, patient's therapy with antibiotics and monoclonal antibodies could cause false positive RBC antibody. Further action needed for better topic covering in future: Except in life threatening condition, reduction of allogenic blood transfusion is recommended. Increase the number of autologous transfusions in all cases when the patient's clinical condition allows. Antigen-free RBC ie universal RBC would be the best choice for transfusion. It is essential to perform extended erythrocyte phenotyping prior to initiation of monoclonal antibodies therapy. As a minimum blood typing for Rh, K, Jka,Jkb, Fya, Fyb and Ss antigens should be done for every patient who is planned to be treated with monoclonal antibodies.Overcoming this problem is very important for patients who are transfusion-dependent or candidates for monoclonal antibody therapy, or candidates for kidney transplantation.

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Section: The Topic Position In Scientific/professional Publicmentioning

confidence: 99%

The role of the Kidd-antibodies in posttransfusion reactions

Nikolić¹,

Čolak²,

Kadija³

et al. 2019

Hosp Pharm Int Multi J

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“…Some of these antibodies recognise red blood cells (RBCs) as well as their intended cancer cell targets and can create considerable havoc in transfusion services when trying to provide compatible blood for transfusion to those patients who are receiving these medications . Anti‐CD38 (daratumumab; DARA) is one example that has been used for a few years now and is FDA approved for use in multiple myeloma patients; unfortunately, it causes panagglutination in serologic tests . The good news is that these serologic reactions are relatively weak (1+ to 2+), and various ways have been reported around the anti‐CD38 panagglutination, enabling elucidation of potentially clinically significant underlying alloantibodies .…”

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confidence: 99%

“…The good news is that these serologic reactions are relatively weak (1+ to 2+), and various ways have been reported around the anti‐CD38 panagglutination, enabling elucidation of potentially clinically significant underlying alloantibodies . These various approaches include the use of dithiothreitol (DTT) and other means to work around this issue and allow more assurances that no potentially clinically significant alloantibodies underly the panagglutination …”

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confidence: 99%

A stressful predicament for blood bankers!

Branch

2020

Transfusion Medicine

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“…Both of these methods may be set up in larger reference laboratories but are not practical for more routine blood transfusion services. Thus, it was found that dithiothreitol (DTT) could be used to treat reference screening and/or panel RBCs and that this DTT treatment would denature the CD38 allowing for subsequent alloantibody investigation . Although this is a method with a history of use in transfusion medicine, DTT treatment at the normal concentration used (0.2 M) can denature additional RBC antigens that could possibly result in missing some clinically significant alloantibodies, especially to high‐prevalence antigens, such those in the Kell blood group system or Cartwright system (i.e., anti‐Yt a ) .…”

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confidence: 99%

“…The article by Velliquette et al paints a picture of the serologic problems that are likely to be encountered when testing patients, not only those receiving anti‐CD38 or anti‐CD47 therapy, but likely what future serology would look like if/when other immunotherapeutics that cross react with RBCs come to fruition . A recurring theme in these reports is that it will be difficult to determine underlying alloantibodies of potential clinical significance in the presence of these therapeutic antibodies.…”

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confidence: 99%