Haematologica (Jun 2009)

Establishment and validation of a standard protocol for the detection of minimal residual disease in B lineage childhood acute lymphoblastic leukemia by flow cytometry in a multi-center setting;

  • Julie Irving,
  • Jenny Jesson,
  • Paul Virgo,
  • Marian Case,
  • Lynne Minto,
  • Lisa Eyre,
  • Nigel Noel,
  • Ulrika Johansson,
  • Marion Macey,
  • Linda Knotts,
  • Margaret Helliwell,
  • Paul Davies,
  • Liam Whitby,
  • David Barnett,
  • Jeremy Hancock,
  • Nick Goulden,
  • Sarah Lawson

DOI
https://doi.org/10.3324/haematol.2008.000414
Journal volume & issue
Vol. 94, no. 6

Abstract

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Minimal residual disease detection, used for clinical management of children with acute lymphoblastic leukemia, can be performed by molecular analysis of antigen-receptor gene rearrangements or by flow cytometric analysis of aberrant immunophenotypes. For flow minimal residual disease to be incorporated into larger national and international trials, a quality assured, standardized method is needed which can be performed in a multi-center setting. We report a four color, flow cytometric protocol established and validated by the UK acute lymphoblastic leukemia Flow minimal residual disease group. Quality assurance testing gave high inter-laboratory agreement with no values differing from a median consensus value by more than one point on a logarithmic scale. Prospective screening of B-ALL patients (n=206) showed the method was applicable to 88.3% of patients. The minimal residual disease in bone marrow aspirates was quantified and compared to molecular data. The combined risk category concordance (minimal residual disease levels above or below 0.01%) was 86% (n=134). Thus, this standardized protocol is highly reproducible between laboratories, sensitive, applicable, and shows good concordance with molecular-based analysis.