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Received on April 15, 2008
Accepted on July 22, 2008
Cancer Diagnostics |
1 Roche Molecular Systems, Pleasanton, CA
2 Institut für Medizinische und Chemische Labordiagnostik, Allgem. öffentliches KH der Elisabethinen, Linz, Austria
3 Hematology Department, University Hospital Basel, Basel, Switzerland
4 Service de Médecine de Laboratoire, Hôpitaux Universitaires de Genève, Genève, Switzerland
5 Munich Leukemia Laboratory, Munich, Germany
* To whom correspondence should be addressed. E-mail: alexander.kohlmann{at}roche.com.
BACKGROUND: Gene expression profiling has the potential to offer consistent, objective diagnostic test results once a standardized protocol has been established. We investigated the robustness, precision, and reproducibility of microarray technology.
METHODS: One hundred sixty individual patient samples representing 11 subtypes of acute and chronic leukemias, myelodysplastic syndromes, and nonleukemia as a control group were centrally collected and diagnosed as part of the daily routine in the Munich Leukemia Laboratory. The custom AmpliChip Leukemia research microarray was used for technical analyses of quadruplicate mononuclear cell lysates in 4 different laboratories in Germany (D), Austria (A), and Switzerland (CH) (the DACH study).
RESULTS: Total-RNA preparations were successfully performed in 637 (99.5%) of 640 cases. Mean differences between pairs of laboratories in the total-RNA yield from the same sample ranged from 0.02 µg to 1.03 µg. Further processing produced 622 successful in vitro transcription reactions (97.6%); the mean differences between laboratories in the cRNA yield from the same sample ranged from 0.40 µg to 6.18 µg. After hybridization to microarrays, a mean of 47.6%, 46.5%, 46.2%, and 46.4% of probe sets were detected as present for the 4 laboratories, with mean signal-intensity scaling factors of 3.1, 3.7, 4.0, and 4.2, respectively. In unsupervised hierarchical cluster and principal component analyses, replicates from the same patient always clustered closely together, with no indications of any association between gene expression profiles due to different operators or laboratories.
CONCLUSIONS: Microarray analysis can be performed with high interlaboratory reproducibility and with comparable quality and high technical precision across laboratories.
The following articles in journals at HighWire Press have cited this article:
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  K. I. Mills, A. Kohlmann, P. M. Williams, L. Wieczorek, W.-m. Liu, R. Li, W. Wei, D. T. Bowen, H. Loeffler, J. M. Hernandez, et al. Microarray-based classifiers and prognosis models identify subgroups with distinct clinical outcomes and high risk of AML transformation of myelodysplastic syndrome Blood, July 30, 2009; 114(5): 1063 - 1072. [Abstract] [Full Text] [PDF]
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 U. Bacher, A. Kohlmann, and T. Haferlach Perspectives of gene expression profiling for diagnosis and therapy in haematological malignancies Brief Funct Genomic Proteomic, May 27, 2009; (2009) elp011v1. [Abstract] [Full Text] [PDF]
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