The p53 gene in pediatric therapy-related leukemia and myelodysplasia

被引:65
作者
Felix, CA
Hosler, MR
Provisor, D
Salhany, K
Sexsmith, EA
Slater, DJ
Cheung, NKV
Winick, NJ
Strauss, EA
Heyn, R
Lange, BJ
Malkin, D
机构
[1] UNIV PENN,SCH MED,DEPT PATHOL & LAB MED,PHILADELPHIA,PA 19104
[2] INDIANA ONCOL HEMATOL CONSULTANTS,INDIANAPOLIS,IN
[3] UNIV TORONTO,HOSP SICK CHILDREN,DEPT PEDIAT,DIV HEMATOL ONCOL,TORONTO,ON,CANADA
[4] MEM SLOAN KETTERING CANC CTR,DEPT PEDIAT,NEW YORK,NY 10021
[5] UNIV TEXAS,SW MED CTR,CHILDRENS MED CTR,CTR CANC & BLOOD DISORDERS,DALLAS,TX
[6] UNIV MICHIGAN,MOTT CHILDRENS HOSP,ANN ARBOR,MI
关键词
D O I
10.1182/blood.V87.10.4376.bloodjournal87104376
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
We investigated the frequency of p53 mutations in 19 pediatric cases of therapy-related leukemia or myelodysplastic syndrome. Eleven children presented with acute myeloid leukemia, one with mixed-lineage leukemia, two with acute lymphoblastic leukemia, and five with myelodysplasia at times ranging from 11 months to 9 years after a primary cancer diagnosis. The primary cancers, which included 11 solid tumors and eight leukemias, were treated with various combinations of DNA topoisomerase II inhibitors, alkylating agents, or irradiation. Leukemic or myelodysplastic marrows were screened for possible mutations by single-strand conformation polymorphism (SSCP) analysis of p53 exons 4 to 8. The only observed mutation was an inherited 2-basepair deletion at codon 209 in exon 6 that would shift the open reading frame, create a premature termination codon, and foreshorten the resultant protein. Prior therapy in this patient included DNA topoisomerase II inhibitors, alkylating agents, and irradiation. The secondary leukemia presented as myelodysplasia with monosomies of chromosomes 5 and 7 and abnormalities of chromosome 17. Although the primary cancer was an embryonal rhabdomyosarcoma and there was a family history of cancer, the case did not fulfill the clinical criteria for Li-Fraumeni syndrome. This study suggests that germline p53 mutations may predispose some children to therapy-related leukemia and myelodysplasia, but that p53 mutations otherwise are infrequent in this setting. (C) 1996 by The American Society of Hematology.
引用
收藏
页码:4376 / 4381
页数:6
相关论文
共 66 条
[1]  
ADDISON C, 1990, ONCOGENE, V5, P423
[2]  
ANDREASSEN A, 1993, CANCER RES, V53, P468
[3]   CELL-DEATH INDUCED BY TOPOISOMERASE INHIBITORS - ROLE OF CALCIUM IN MAMMALIAN-CELLS [J].
BERTRAND, R ;
KERRIGAN, D ;
SARANG, M ;
POMMIER, Y .
BIOCHEMICAL PHARMACOLOGY, 1991, 42 (01) :77-85
[4]  
BIRCH JM, 1994, CANCER RES, V54, P1298
[5]  
BRUGIERES L, 1993, CANCER RES, V53, P452
[6]   DNA TOPOISOMERASE-TRAPPING ANTITUMOR DRUGS [J].
CAPRANICO, G ;
ZUNINO, F .
EUROPEAN JOURNAL OF CANCER, 1992, 28A (12) :2055-2060
[7]  
CARBONE D, 1991, ONCOGENE, V6, P1691
[8]  
CHEN GL, 1984, J BIOL CHEM, V259, P3560
[9]   THYMOCYTE APOPTOSIS INDUCED BY P53-DEPENDENT AND INDEPENDENT PATHWAYS [J].
CLARKE, AR ;
PURDIE, CA ;
HARRISON, DJ ;
MORRIS, RG ;
BIRD, CC ;
HOOPER, ML ;
WYLLIE, AH .
NATURE, 1993, 362 (6423) :849-852
[10]   WHEN GOOD ENZYMES GO BAD - CONVERSION OF TOPOISOMERASE-II TO A CELLULAR TOXIN BY ANTINEOPLASTIC DRUGS [J].
CORBETT, AH ;
OSHEROFF, N .
CHEMICAL RESEARCH IN TOXICOLOGY, 1993, 6 (05) :585-597