Samenvatting
Flow cytometric minimal residual disease (MRD) monitoring could become more powerful if directed towards the disease-maintaining leukemic stem cell (LSC) compartment. Using a cohort of 48 children with B-lineage acute lymphoblastic leukemia (ALL), we sought the newly proposed candidate-LSC population, CD34+CD38lowCD19+, at presentation and in end of induction bone marrow samples. We identified the candidate LSC population in 60% of diagnostic samples and its presence correlated with expression of CD38, relative to that of normal B-cell progenitors. In addition, the candidate LSC was not detectable in all MRD positive samples. The absence of the population in 40% of diagnostic and 40% of MRD positive samples does not support the use of this phenotype as a generic biomarker to track LSCs and suggests that this phenotype may be an artifact of CD38 underexpression rather than a biologically distinct LSC population.
Originele taal-2 | Engels |
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Pagina's (van-tot) | 679-683 |
Aantal pagina's | 5 |
Tijdschrift | Haematologica |
Volume | 95 |
Nummer van het tijdschrift | 4 |
DOI's | |
Status | Gepubliceerd - apr. 2010 |
Extern gepubliceerd | Ja |