Fifteen years of external quality assessment in leukemia/lymphoma immunophenotyping in The Netherlands and Belgium: A way forward

Fifteen years of external quality assessment in leukemia/lymphoma immunophenotyping in The Netherlands and Belgium: A way forward

In 1985, external quality assurance was initiated in the Netherlands to reduce the between‐laboratory variability of leukemia/lymphoma immunophenotyping and to improve diagnostic conclusions. This program consisted of regular distributions of test samples followed by biannual plenary participant mee...

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Veröffentlicht in:Cytometry. Part B, Clinical cytometry Clinical cytometry, 2016-05, Vol.90 (3), p.267-278
Hauptverfasser: Preijers, Frank W. M. B., van der Velden, Vincent H. J., Preijers, Tim, Brooimans, Rik A., Marijt, Erik, Homburg, Christa, van Montfort, Kees, Gratama, Jan W.
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Sprache:eng
Schlagworte:
Acute Disease
Belgium
external quality control
flow cytometry
Flow Cytometry - methods
Humans
immunophenotyping
Immunophenotyping - methods
leukemia
Leukemia - pathology
lymphoma
Lymphoma - diagnosis
Lymphoma - pathology
Netherlands
Quality Control
Retrospective Studies
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container_end_page 278
container_issue 3
container_start_page 267
container_title Cytometry. Part B, Clinical cytometry
container_volume 90
creator Preijers, Frank W. M. B.
van der Velden, Vincent H. J.
Preijers, Tim
Brooimans, Rik A.
Marijt, Erik
Homburg, Christa
van Montfort, Kees
Gratama, Jan W.
description In 1985, external quality assurance was initiated in the Netherlands to reduce the between‐laboratory variability of leukemia/lymphoma immunophenotyping and to improve diagnostic conclusions. This program consisted of regular distributions of test samples followed by biannual plenary participant meetings in which results were presented and discussed. A scoring system was developed in which the quality of results was rated by systematically reviewing the pre‐analytical, analytical, and post‐analytical assay stages using three scores, i.e., correct (A), minor fault (B), and major fault (C). Here, we report on 90 consecutive samples distributed to 40–61 participating laboratories between 1998 and 2012. Most samples contained >20% aberrant cells, mainly selected from mature lymphoid malignancies (B or T cell) and acute leukemias (myeloid or lymphoblastic). In 2002, minimally required monoclonal antibody (mAb) panels were introduced, whilst methodological guidelines for all three assay stages were implemented. Retrospectively, we divided the study into subsequent periods of 4 (“initial”), 4 (“learning”), and 7 years (“consolidation”) to detect “learning effects.” Uni‐ and multivariate models showed that analytical performance declined since 2002, but that post‐analytical performance improved during the entire period. These results emphasized the need to improve technical aspects of the assay, and reflected improved interpretational skills of the participants. A strong effect of participant affiliation in all three assay stages was observed: laboratories in academic and large peripheral hospitals performed significantly better than those in small hospitals. © 2015 International Clinical Cytometry Society
doi_str_mv 10.1002/cyto.b.21266
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subjects Acute Disease
Belgium
external quality control
flow cytometry
Flow Cytometry - methods
Humans
immunophenotyping
Immunophenotyping - methods
leukemia
Leukemia - pathology
lymphoma
Lymphoma - diagnosis
Lymphoma - pathology
Netherlands
Quality Control
Retrospective Studies
title Fifteen years of external quality assessment in leukemia/lymphoma immunophenotyping in The Netherlands and Belgium: A way forward
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