Characterization of fusion partner genes in 114 patients with de novo acute myeloid leukemia and MLL rearrangement

被引:0
|
作者
L-y Shih
D-c Liang
J-f Fu
J-h Wu
P-n Wang
T-l Lin
P Dunn
M-c Kuo
T-c Tang
T-h Lin
C-l Lai
机构
[1] Chang Gung Memorial Hospital,Division of Hematology
[2] School of Medicine,Oncology, Department of Internal Medicine
[3] Chang Gung University,Division of Pediatric Hematology
[4] Mackay Memorial Hospital,Oncology
来源
Leukemia | 2006年 / 20卷
关键词
acute myeloid leukemia; rearrangement; -fusion transcript; partner gene; partial tandem duplication;
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学科分类号
摘要
The fusion transcripts of MLL rearrangement [MLL(+)] in acute myeloid leukemia (AML) and their clinicohematologic correlation have not be well characterized in the previous studies. We used Southern blot analysis to screen MLL(+) in de novo AML. Reverse transcriptase-polymerase chain reaction was used to detect the common MLL fusion transcripts. cDNA panhandle PCR was used to identify infrequent or unknown MLL partner genes. MLL(+) was identified in 114 (98 adults) of 988 AML patients. MLL fusion transcripts comprised of 63 partial tandem duplication of MLL (MLL-PTD), 14 MLL-AF9, 9 MLL-AF10, 9 MLL-ELL, 8 MLL-AF6, 4 MLL-ENL and one each of MLL-AF1, MLL-AF4, MLL-MSF, MLL-LCX, MLL-LARG, MLL-SEPT6 and MLL-CBL. The frequency of MLL-PTD was 7.1% in adults and 0.9% in children (P<0.001). 11q23 abnormalities were detected in 64% of MLL/t11q23 and in none of MLL-PTD by conventional cytogenetics. There were no differences in remission rate, event-free survival and overall survival between adult MLL-PTD and MLL/t11q23 groups. Adult patients had a significantly poorer outcome than children. The present study showed that cDNA panhandle PCR can identify all rare or novel MLL partner genes. MLL-PTD was rare in childhood AML. MLL(+) adults had a poor outcome with no difference in survival between MLL-PTD and MLL/t11q23 groups.
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页码:218 / 223
页数:5
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