Critical Care Clinical Trial
Official title:
Cell-derived Microparticles in Red Blood Cell (RBC) Concentrates, and Their Potential Impact on Outcomes of Transfused Patients in Critical Care: a Prospective Multicentre National Cohort Study of Patients Included in the ABLE Trial
During storage, red blood cells (RBCs) undergo changes collectively termed "Storage lesions". these changes may have an impact of the outcomes of transfused patients. One of these changes is the release of microparticles by RBCs and other blood cells types. The aim of the study is to (1) quantify red cell- and platelet-derived microparticles in RBC concentrates, and (2) evaluate the impact of transfused microparticles (MPs) on survival and post-transfusion complications in critical care patients participating in the ABLE trial (ISRCTN44878718).
During conservation of red blood cell concentrates, red blood cells (RBCs) undergo
biochemical and morphological changes that have been well described, and are collectively
termed " storage lesions ". The exact effects of these lesions in terms of beneficial or
deleterious implications in the recipient remain to be elucidated. However, several
retrospective studies in targeted populations suggest that an increase in the duration of
RBC conservation could lead to an increase in morbidity and mortality in transfused
patients. The multicenter, prospective trial ABLE (Age of Blood Evaluation, ISRCTN44878718)
aimed to evaluate in a randomised clinical trial, the impact of the age of transfused RBC
concentrates on several outcomes in critical care patients.
Among the modifications that RBCs undergo during storage, the generation of microparticles
from red blood cellsRBCs or residual platelets present in the blood concentrate has never
been evaluated in a prospective clinical study. It has been reported that the number of red
cell-derived microparticles (RMPs) present in stored blood increases with storage duration.
In vivo, microparticles MPs appear to be increasingly involved in disease processes, notably
due to their pro-inflammatory and pro-coagulant effects. Furthermore, it has been shown that
the antigens of the Rhesus group are expressed on the RBC derived microparticles, and the
investigative team has shown that microparticles derived from elsewhere (endothelial cells)
are capable of activating cells which are important in the induction of immune responses
(dendritic cells). Thus, transfusing red blood cell derived microparticles could participate
in post-transfusional alloimmunization which may also be evaluated in this study.
The aim of the IMIB study is to (1) quantify red cell- and platelet-derived microparticles
MPs in RBC concentrates, and (2) evaluate the impact of the quantity of transfused
microparticles (MPs) on survival and several outcomes in the patients enrolled in the ABLE
trial in France.
Other aims are to investigate the relationship between the number of microparticles in RBC
units and (1) the age of RBC, (2) donors characteristics, (3) the procedures used to prepare
the blood products (to define a potential new "lesion storage" marker).
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