Publication Date:
2007-11-16
Description:
The MILE (Microarray Innovations in LEukemia) study has previously shown that gene expression signatures associated with initial leukaemia classifier (LCver7) give an overall cross-validation accuracy of 〉95% for distinct sub-classes of pediatric and adult leukemias. However, only 50% of the 174 MDS samples in the whole-genome microarray analysis (Stage 1) of the MILE study were correctly identified; the remainder showed AML-like or non-leukemia-like gene profiles. An external morphological review (DB & HL) according to FAB and WHO criteria, of the 174 slides was performed independently (blind) which resulted in 6 samples being reclassified as AML and 4 non-leukemia cases excluded from the study. A recently improved, hierarchical based algorithm correctly identified 100% of the confirmed MDS cases. In this study, using LCver7, the confirmed 164 samples had 50% MDS classifications (Class 17), 23.8% non-leukemia classifications (Class 18), and 22.6% AML classifications (Classes 13 or 14) with the remaining 3.7% having a classification tie between 2 or 3 Classes (due to low confidence). No 5q- syndrome patients had an AML call, whilst 68.3% of RAEB2 patients had an AML classification and none were Class 18. Similarly, 95.6% of Low IPSS patients were classified as Class 17 or 18, whilst all patients (n=5) with High IPSS had an AML call. The classification was independent of blast cells: 10.2% of Class 18 calls had 〉5% blasts; 28.2% of AML-like cases had
Print ISSN:
0006-4971
Electronic ISSN:
1528-0020
Topics:
Biology
,
Medicine
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