Complement Inhibition with C1 Esterase Inhibitor Allowed Successful Transfusion of Antigen Mismatched Packed Red Blood Cells : A Case Report

▪ Hemolytic transfusion reactions (HTRs) occur after donor packed red blood cell (PRBCs) transfusions with antigenic differences including the major antigen system, ABO, as well as minor antigen systems such as Rh, Kell, Duffy, Kidd, JH, and U. These reactions are classified as acute if they occur w...

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Published in:Blood 2016-12, Vol.128 (22), p.3843-3843
Main Authors: Warner, Eiran, Broome, Catherine
Format: Article
Language:English
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Summary:▪ Hemolytic transfusion reactions (HTRs) occur after donor packed red blood cell (PRBCs) transfusions with antigenic differences including the major antigen system, ABO, as well as minor antigen systems such as Rh, Kell, Duffy, Kidd, JH, and U. These reactions are classified as acute if they occur within the first 24 hours or delayed if occurring after 24 hours. Antigen mismatched transfusions activate the classical pathway of complement leading to intravascular hemolysis via C5b-9 and extravascular hemolysis via C3b mediated phagocytosis in the spleen and liver (Stowell et al. Clin Devel Immunol 2012).In addition to laboratory evidence of hemolysis and increased antibody titers, patients can experience a wide range of clinical symptoms including fever, rash, chest, abdomen or back pain, signs of hemodynamic instability and death. (Strobel. Trans Med & Hemo 2008) Mouse models have demonstrated that the inhibition of complement receptor 1 resulted in increased survival of mismatched transfused RBCs (Yazdanbakhsh et al. Blood 2003). The terminal complement inhibitor, eculizumab, has been used to successfully rescue a patient after a severe ABO incompatible hemolytic transfusion reaction (Weinstock et al. Transfusion 2015). Based on these data, we postulated that the prophylactic administration of a C1 esterase inhibitor would interrupt activation of the classical complement pathway, mitigating a hemolytic transfusion reaction to antigen mismatched PRBCs. A 50 year old African American male with widely metastatic prostate cancer presented with a hemoglobin (Hgb) of 5.1 g/dL and a platelet count of 39K/uL. His cytopenias had progressively worsened over the past 6 months from a baseline Hgb of 12 gm/dL and platelet count of 222 K/uL, and were secondary to bone metastases and prior spinal radiation. Thirty days prior to presentation, he received one unit of PRBCs at an outside institution for a Hgb of 7.0 g/dL. Due to worsening Hgb and clinical symptoms, a direct antiglobulin test (DAT) was obtained 21 days after the transfusion. It was noted to be positive for C3d suggesting a delayed hemolytic transfusion reaction. Upon type and cross match he was found to be O+ with new antibodies to Jka and U. A single compatible unit of PRBCs was identified and transfused. His Hgb increased from 4.5 g/dL to 5.9 g/dL with transfusion. His Hgb remained near 5g/dL over the next week however, he remained very symptomatic. There were no additional matched PRBCS available for tra
ISSN:0006-4971
1528-0020
DOI:10.1182/blood.V128.22.3843.3843