Survival of Donor Leukocyte Subpopulations in Immunocompetent Transfusion Recipients: Frequent Long-Term Microchimerism in Severe Trauma Patients
Open Access
- 1 May 1999
- journal article
- Published by American Society of Hematology in Blood
- Vol. 93 (9), 3127-3139
- https://doi.org/10.1182/blood.v93.9.3127
Abstract
We recently reported detection of a transient increase in circulating donor leukocytes (WBCs) in immunocompetent recipients 3 to 5 days posttransfusion (tx) (Blood 85:1207, 1995). We have now characterized survival kinetics of specific donor WBC subsets in additional tx populations. Eight female elective surgery patients (pts) were sampled pre-tx and on days 1, 3, 5, 7, and 14 post-tx. Ten female trauma pts transfused with a total of 4 to 18 U of relatively fresh red blood cells were sampled up to 1.5 years post-tx. WBC subsets from frozen whole blood were isolated using CD4, CD8 (T cell), CD15 (myeloid), and CD19 (B cell) antibody-coated magnetic beads. Donor WBCs were counted by quantitative polymerase chain reaction (PCR) of male-specific sex determining region (SRY) sequences. PCR HLA typing and mixed leukocyte reaction (MLR) between recipient and donor WBCs were performed on two of the trauma tx recipients who had long-term chimerism of donor cells post-tx. In 6 of 8 female surgery pts, circulating CD4+ male donor cells peaked at day 3 or 5 (0.01 to 1 cell/μL), followed by clearance by day 14. In 7 of 10 female trauma pts, we observed multilineage persistence of male donor WBCs (CD4, CD8, CD15, CD19) for 6 months to 1.5 years post-tx at concentrations of 10 to 100 cells/μL. In 2 trauma recipients studied, MLR showed no, or very low, response to WBC of the single donor implicated as the source of microchimerism by HLA typing. Establishment of long-term multilineage chimerism in trauma recipients is probably caused by engraftment of donor stem cells and mutual tolerance between recipient and donor leukocytes. A better understanding of factors determining clearance versus chimerism of transfused leukocytes is critical to prevention of alloimmunization and transfusion-induced graft-versus-host disease, and, potentially, to induction of tolerance for transplantation.Keywords
This publication has 55 references indexed in Scilit:
- Posttraumatic Lymphocyte ResponsePublished by Wolters Kluwer Health ,1998
- Neonatal Tolerance Revisited: Turning on Newborn T Cells with Dendritic CellsScience, 1996
- HUMAN PERIPHERAL MONONUCLEAR CELLS DO NOT SHOW PROINFLAMMATORY PATTERNS OF CYTOKINE TRANSCRIPTION IN EARLY TRAUMAShock, 1995
- TRAUMA-HEMORRHAGE CAUSES PROLONGED DEPRESSION IN CELLULAR IMMUNITYShock, 1995
- Hematopoietic stem and progenitor cells from blood: emerging uses for new components for transfusionTransfusion, 1995
- Graft-versus-Host Disease Associated with Transfusion of Blood from Unrelated HLA-Homozygous DonorsNew England Journal of Medicine, 1993
- THE TIME COURSE OF CELL-MEDIATED LYMPHOLYSIS IN RAT HEPATIC ALLOGRAFT RECIPIENTS PRETREATED WITH A SINGLE DONOR-SPECIFIC BLOOD TRANSFUSIONTransplantation, 1992
- A gene from the human sex-determining region encodes a protein with homology to a conserved DNA-binding motifNature, 1990
- Use of leucocyte‐poor blood components and HLA‐matched‐platelet donors to prevent HLA alloimmunizationBritish Journal of Haematology, 1986
- Blood transfusion-induced suppression of cellular immunity in manHuman Immunology, 1980