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Does expression of different EWS chimeric transcripts define clinically distinct risk groups of Ewing tumor patients?

被引:227
作者
Zoubek, A
DockhornDworniczak, B
Delattre, O
Christiansen, H
Niggli, F
GattererMenz, I
Smith, TL
Jurgens, H
Gadner, H
Kovar, H
机构
[1] ST ANNA CHILDRENS HOSP,CHILDRENS CANC RES INST,A-1090 VIENNA,AUSTRIA
[2] UNIV VIENNA,DEPT MED COMP SCI,SECT CLIN BIOMETR,VIENNA,AUSTRIA
[3] UNIV MUNSTER,GERHARD DOMAGK INST PATHOL,W-4400 MUNSTER,GERMANY
[4] UNIV MUNSTER,DEPT PEDIAT HEMATOL & ONCOL,W-4400 MUNSTER,GERMANY
[5] UNIV GIESSEN,DEPT PEDIAT ONCOL & HEMATOL,W-6300 GIESSEN,GERMANY
[6] INST CURIE,LAB GENET TUMEURS,PARIS,FRANCE
[7] UNIV ZURICH,CHILDRENS HOSP,ZURICH,SWITZERLAND
来源
JOURNAL OF CLINICAL ONCOLOGY | 1996年 / 14卷 / 04期
关键词
D O I
10.1200/JCO.1996.14.4.1245
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose: Because of the high heterogeneity of EWS gene fusions with FLI1 and ERG genes due to variable chromosomal breakpoint locations in Ewing tumors (ET) (14 different chimeric transcripts identified so far), we evaluated the clinical impact of the expression of diverse fusion transcripts in ET patients. Patients and Methods: In a European multicenter study, 147 ET were analyzed by reverse-transciptase polymerase chain reaction (RT-PCR) and the molecular data statistically compared with all clinical data available. Results: Most rumors expressed chimeric transcripts with fusion of EWS exon 7 to FLI1 exon 6 (75 of 147) (type I) or five (39 of 147) and EWS exon 10 to FLI1 exon 5 (eight of 147) or 6 (five of 147). In five cases, chimerism between EWS exon 9 and FLI1 exons 4 and EWS exon 7 and FLI1 exon 7 or 8 was observed. Fifteen cases of EWS-ERG rearrangement were identified, In 85 of these patients treated in the European Cooperative Ewing Sarcoma Studies, molecular results were analyzed in comparison to age, sex, tumor localization, tumor volume, and disease extension. No significant correlation between the various fusion types and these features were observed. Relapse-free survival (RFS) for the 31 patients with localized disease and fusion type I tended to be longer compared with the 24 patients with localized tumors bearing other chimeric transcripts (P = .04). (C) 1996 by American Society of Clinical Oncology. Conclusion: Results suggest a possible advantage in RFS for patients with localized disease and fusion type I transcripts, although this will require prospective validation with a larger number of patients and longer follow-up periods.
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页码:1245 / 1251
页数:7
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