Erythrocyte-derived ectosomes have immunosuppressive properties

Several clinical studies have suggested that blood transfusions are immunosuppressive. Whereas there have been reports describing immunosuppression induced by leukocytes or fragments thereof, the possibility that microparticles, released by erythrocytes during storage, are also involved was not inve...

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Veröffentlicht in:Journal of leukocyte biology 2008-11, Vol.84 (5), p.1316-1325
Hauptverfasser: Sadallah, Salima, Eken, Ceylan, Schifferli, Jürg A.
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container_title Journal of leukocyte biology
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creator Sadallah, Salima
Eken, Ceylan
Schifferli, Jürg A.
description Several clinical studies have suggested that blood transfusions are immunosuppressive. Whereas there have been reports describing immunosuppression induced by leukocytes or fragments thereof, the possibility that microparticles, released by erythrocytes during storage, are also involved was not investigated. We present evidence here that such microparticles have all the properties of ectosomes including size, the presence of a lipid membrane, and the specific sorting of proteins. These erythrocyte‐derived ectosomes (E‐ecto) fixed C1q, which was followed by activation of the classical pathway of complement with binding of C3 fragments. Similarly to ectosomes released by PMN, they express phosphatidylserine on their surface membrane, suggesting that they may react with and down‐regulate cells of the immune system. In vitro, they were taken up by macrophages, and they significantly inhibited the activation of these macrophages by zymosan A and LPS, as shown by a significant drop in TNF‐α and IL‐8 release (respectively, 80% and 76% inhibitions). In addition, the effect of E‐ecto was not transient but lasted for at least 24 h. In sum, E‐ecto may interfere with the innate immune system/inflammatory reaction. Therefore, E‐ecto transfused with erythrocytes may account for some of the immunosuppressive properties attributed to blood transfusions.
doi_str_mv 10.1189/jlb.0108013
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Whereas there have been reports describing immunosuppression induced by leukocytes or fragments thereof, the possibility that microparticles, released by erythrocytes during storage, are also involved was not investigated. We present evidence here that such microparticles have all the properties of ectosomes including size, the presence of a lipid membrane, and the specific sorting of proteins. These erythrocyte‐derived ectosomes (E‐ecto) fixed C1q, which was followed by activation of the classical pathway of complement with binding of C3 fragments. Similarly to ectosomes released by PMN, they express phosphatidylserine on their surface membrane, suggesting that they may react with and down‐regulate cells of the immune system. In vitro, they were taken up by macrophages, and they significantly inhibited the activation of these macrophages by zymosan A and LPS, as shown by a significant drop in TNF‐α and IL‐8 release (respectively, 80% and 76% inhibitions). In addition, the effect of E‐ecto was not transient but lasted for at least 24 h. In sum, E‐ecto may interfere with the innate immune system/inflammatory reaction. 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Whereas there have been reports describing immunosuppression induced by leukocytes or fragments thereof, the possibility that microparticles, released by erythrocytes during storage, are also involved was not investigated. We present evidence here that such microparticles have all the properties of ectosomes including size, the presence of a lipid membrane, and the specific sorting of proteins. These erythrocyte‐derived ectosomes (E‐ecto) fixed C1q, which was followed by activation of the classical pathway of complement with binding of C3 fragments. Similarly to ectosomes released by PMN, they express phosphatidylserine on their surface membrane, suggesting that they may react with and down‐regulate cells of the immune system. In vitro, they were taken up by macrophages, and they significantly inhibited the activation of these macrophages by zymosan A and LPS, as shown by a significant drop in TNF‐α and IL‐8 release (respectively, 80% and 76% inhibitions). In addition, the effect of E‐ecto was not transient but lasted for at least 24 h. In sum, E‐ecto may interfere with the innate immune system/inflammatory reaction. 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subjects Animals
Annexin A5 - physiology
Antibodies, Monoclonal
Blood Transfusion
complement
Complement Activation
Complement C1q - physiology
cytokines
Erythrocytes - cytology
Erythrocytes - immunology
Erythrocytes - physiology
Erythrocytes - ultrastructure
Flow Cytometry
Humans
Macrophages - physiology
Mice
Microscopy, Confocal
Microscopy, Electron
monocyte/macrophages
Neutrophils - immunology
Neutrophils - physiology
phagocytosis
Protein Binding
Subcellular Fractions - immunology
Subcellular Fractions - physiology
Subcellular Fractions - ultrastructure
title Erythrocyte-derived ectosomes have immunosuppressive properties
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