Detailed immunophenotyping of B‐cell precursors in regenerating bone marrow of acute lymphoblastic leukaemia patients: implications for minimal residual disease detection

Summary Flow cytometric detection of minimal residual disease ( MRD ) in children with B‐cell precursor acute lymphoblastic leukaemia ( BCP ‐ ALL ) requires immunophenotypic discrimination between residual leukaemic cells and B‐cell precursors ( BCP s) which regenerate during therapy intervals. In this study, EuroFlow‐based 8‐colour flow cytometry and innovative analysis tools were used to first characterize the immunophenotypic maturation of normal BCP s in bone marrow ( BM ) from healthy children, resulting in a continuous multiparametric pathway including transition stages. This pathway was subsequently used as a reference to characterize the immunophenotypic maturation of regenerating BCP s in BM from children treated for BCP ‐ ALL . We identified pre‐B‐I cells that expressed low or dim CD34 levels, in contrast to the classical CD34 high pre‐B‐I cell immunophenotype. These CD34 −dim pre‐B‐I cells were relatively abundant in regenerating BM (11–85% within pre‐B‐I subset), while hardly present in healthy control BM (9–13% within pre‐B‐I subset; P  =   0·0037). Furthermore, we showed that some of the BCP ‐ ALL diagnosis immunophenotypes (23%) overlapped with CD34 −dim pre‐B‐I cells. Our results indicate that newly identified CD34 −dim pre‐B‐I cells can be mistaken for residual BCP ‐ ALL cells, potentially resulting in false‐positive MRD outcomes. Therefore, regenerating BM , in which CD34 −dim pre‐B‐I cells are relatively abundant, should be used as reference frame in flow cytometric MRD measurements.