Transfusion of target antigens to preimmunized recipients: a new mechanism in transfusion-related acute lung injury

Author:

Bayat Behnaz1ORCID,Nielsen Kaspar René2,Bein Gregor1ORCID,Traum Annalena1,Burg-Roderfeld Monika3,Sachs Ulrich J.1ORCID

Affiliation:

1. Institute for Clinical Immunology and Transfusion Medicine, Justus Liebig University, Giessen, Germany;

2. Clinical Immunology, Aalborg University Hospital, Aalborg, Denmark; and

3. Faculty of Biology and Chemistry, Fresenius University of Applied Sciences, Idstein, Germany

Abstract

Abstract Transfusion-related lung injury (TRALI) is a serious side effect of blood transfusion. Exclusion of antibody carriers from the donor pool has significantly decreased the number of cases, but TRALI remains the leading cause of transfusion-related morbidity and mortality in industrialized countries. Here, we show that proteins released from donor cells during processing of blood components are capable of inducing a new type of reverse TRALI when transfused to preimmunized recipients. First, we show that soluble neutrophil surface protein CD177 in complex with proteinase 3 (sCD177/PR3) is not only present in human plasma but also in packed red blood cell (PRBC) supernatant. Filtration or storage enhances the concentration of sCD177/PR3 in PRBCs. Second, we show that sCD177/PR3 specifically binds to PECAM-1 on stimulated (but not on unstimulated) endothelial cells (ECs). Third, we provide evidence that the sCD177/PR3/PECAM-1 complex is functional. In the presence of monoclonal or human antibodies against CD177 or PR3, ECs produce reactive oxygen species and become apoptotic. Albumin flux through an EC monolayer increases significantly whenever antibodies and the cognate antigens are present. Finally, we describe a clinical case in which anti-CD177 present in a transfusion recipient precipitated TRALI after the transfusion of CD177-positive, but not CD177-negative, PRBCs. In conclusion, we introduce a new TRALI mechanism based on the specific binding of transfused, soluble antigens to activated ECs in preimmunized recipients. We suggest that further studies and clinical work-up of TRALI should also include antibody investigation of the recipient.

Publisher

American Society of Hematology

Subject

Hematology

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