Early CD3+/CD15+ peripheral blood leukocyte chimerism patterns correlate with long-term engraftment in non-malignant hematopoietic SCT

被引:0
|
作者
T G Ketterl
M Flesher
R Shanley
W Miller
机构
[1] Internal Medicine/Pediatrics,
[2] University of Minnesota,undefined
[3] Pediatric Blood and Marrow Transplant,undefined
[4] University of Minnesota,undefined
[5] Biostatistics and Bioinformatics Core,undefined
[6] Masonic Cancer Center,undefined
[7] University of Minnesota,undefined
来源
Bone Marrow Transplantation | 2014年 / 49卷
关键词
non-malignant; transplant; chimerism; CD3+; CD15+; engraftment;
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摘要
Following hematopoietic SCT (HSCT) for non-malignant disorders (NMDs) variable donor chimerism among lympho-hematopoietic lines may be observed. We retrospectively evaluated early post-HSCT, lineage-sorted (CD3+ and CD15+) peripheral blood leukocyte chimerism data to characterize patterns and assess for association with long-term CD15+ engraftment. ‘Early’ was defined as the first value obtained between days +14 and +42, ‘late’ as the last recorded value after day +90. ‘High’ donor chimerism was defined as ⩾80% on either fraction at all time-points. Patients were classified into four subgroups with respect to early CD3+/CD15+ chimerism patterns (high/low) then analyzed for long-term CD15+ chimerism status. A total of 135 transplants were evaluable, with all three time-points available in 97. Underlying disease, graft source, patient age and conditioning intensity varied. ‘Split’ early chimerism (discordant high/low CD3+/CD15+ status) was common. Multivariable analysis revealed strong association between conditioning regimen and primary disease on early CD3+/CD15+ chimerism patterns and a dominant predictive effect of early CD15+ chimerism on long-term CD15+ donor engraftment (observed at median day +365). These data may guide real-time clinician decisions (restraint vs intervention, when available) when faced with unfavorable or unusual early lympho-hematopoietic chimerism patterns following HSCT for NMD.
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页码:572 / 575
页数:3
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