Literature DB >> 33657208

Rapid clearance of storage-induced microerythrocytes alters transfusion recovery.

Camille Roussel1,2,3,4, Alexandre Morel1,2,5, Michaël Dussiot1,2, Mickaël Marin2,3,4, Martin Colard1,2, Aurélie Fricot-Monsinjon2,3,4, Anaïs Martinez1,2, Charlotte Chambrion2,3,4, Benoît Henry2,3,4, Madeleine Casimir1,2, Geoffroy Volle2,3,4, Mallorie Dépond2,3,4, Safi Dokmak6, François Paye7, Alain Sauvanet6, Caroline Le Van Kim2,3,4, Yves Colin2,3,4, Sonia Georgeault8, Philippe Roingeard8,9, Steven L Spitalnik10, Papa Alioune Ndour2,3,4, Olivier Hermine1,2,5, Eldad A Hod10, Pierre A Buffet2,3,4,11, Pascal Amireault1,2,3,4.   

Abstract

Permanent availability of red blood cells (RBCs) for transfusion depends on refrigerated storage, during which morphologically altered RBCs accumulate. Among these, a subpopulation of small RBCs, comprising type III echinocytes, spheroechinocytes, and spherocytes and defined as storage-induced microerythrocytes (SMEs), could be rapidly cleared from circulation posttransfusion. We quantified the proportion of SMEs in RBC concentrates from healthy human volunteers and assessed correlation with transfusion recovery, investigated the fate of SMEs upon perfusion through human spleen ex vivo, and explored where and how SMEs are cleared in a mouse model of blood storage and transfusion. In healthy human volunteers, high proportion of SMEs in long-stored RBC concentrates correlated with poor transfusion recovery. When perfused through human spleen, 15% and 61% of long-stored RBCs and SMEs were cleared in 70 minutes, respectively. High initial proportion of SMEs also correlated with high retention of RBCs by perfused human spleen. In the mouse model, SMEs accumulated during storage. Transfusion of long-stored RBCs resulted in reduced posttransfusion recovery, mostly due to SME clearance. After transfusion in mice, long-stored RBCs accumulated predominantly in spleen and were ingested mainly by splenic and hepatic macrophages. In macrophage-depleted mice, splenic accumulation and SME clearance were delayed, and transfusion recovery was improved. In healthy hosts, SMEs were cleared predominantly by macrophages in spleen and liver. When this well-demarcated subpopulation of altered RBCs was abundant in RBC concentrates, transfusion recovery was diminished. SME quantification has the potential to improve blood product quality assessment. This trial was registered at www.clinicaltrials.gov as #NCT02889133.
© 2021 by The American Society of Hematology.

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Year:  2021        PMID: 33657208      PMCID: PMC8085482          DOI: 10.1182/blood.2020008563

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


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