UNBALANCED TRANSLOCATION T(5-17) IN AN ATYPICAL ACUTE PROMYELOCYTIC LEUKEMIA

被引：25

作者：

BRUNEL, V

SAINTY, D

CARBUCCIA, N

ARNOULET, C

COSTELLO, R

MOZZICONACCI, MJ

SIMONETTI, J

COIGNET, L

GABERT, J

STOPPA, AM

BIRG, F

LAFAGEPOCHITALOFF, M

机构：

[1] INST J PAOLI I CALMETTES,DEPT BIOL,INSERM,U119,F-13009 MARSEILLE,FRANCE

[2] INST J PAOLI I CALMETTES,DIV HEMATOL,MARSEILLE,FRANCE

来源：

GENES CHROMOSOMES & CANCER | 1995年 / 14卷 / 04期

关键词：

D O I：

10.1002/gcc.2870140410

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Acute promyelocytic leukemia (APL; M3 in the FAB classification) is specifically associated with the t(15;17)(q23;q12) and the consequent formation of a PML/RARA fusion gene. A few cases of APL with a t(11;17)(q23;q12) and a PLZF/RARA fusion gene have recently been reported. In addition, a new variant, t(5;17)(q32;q12), with a RARA rearrangement was described in a child with atypical APL. We report an unbalanced der(5)t(5;17) in an atypical APL case showing unusual dysgranulopoiesis and some M2 features. The breakpoints were difficult to localize precisely on chromosome 5, because the translocation may have occurred on a previous del(5q). The karyotype also showed del(8q) and multiple double-minutes (dmin). Molecular studies evidenced RARA rearrangement but showed neither PML rearrangement nor PML/RARA fusion. Fluorescence in situ hybridization revealed that the dmin were of chromosome 8 origin and that they accounted for the MYC amplification observed in Southern blots. The patient did very poorly despite chemotherapy and all-trans retinoic acid (ATRA) treatment. Thus, the t(5;17) could represent a second type of variant translocation in APL that, like the disease associated with t(11;17), does not seem to respond to ATRA therapy. Whereas RARA rearrangement appears sufficient for an APL-like phenotype, it seems that the presence of a classical PML/RARA is required for typical APL with response to ATRA.

引用

页码：307 / 312

页数：6

共 22 条

[1] AGADIR A, 1994, CELL MOL BIOL, V40, P263
[2] BIONDI A, 1992, BLOOD, V80, P492
[3] BORROW J, 1993, GENES CHROMOSOM CANC, V9, P234
[4] GENE AMPLIFICATION AND TUMOR PROGRESSION
BRISON, O
[J]. BIOCHIMICA ET BIOPHYSICA ACTA, 1993, 1155 (01) : 25 - 41
[5] REARRANGEMENTS OF THE RETINOIC ACID RECEPTOR-ALPHA AND PROMYELOCYTIC LEUKEMIA ZINC-FINGER GENES RESULTING FROM T(11 17)(Q23 Q21) IN A PATIENT WITH ACUTE PROMYELOCYTIC LEUKEMIA
CHEN, SJ
ZELENT, A
TONG, JH
YU, HQ
WANG, ZY
DERRE, J
BERGER, R
WAXMAN, S
CHEN, Z
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1993, 91 (05) : 2260 - 2267
[6] FUSION BETWEEN A NOVEL KRUPPEL-LIKE ZINC FINGER GENE AND THE RETINOIC ACID RECEPTOR-ALPHA LOCUS DUE TO A VARIANT T(11,17) TRANSLOCATION ASSOCIATED WITH ACUTE PROMYELOCYTIC LEUKEMIA
CHEN, Z
BRAND, NJ
CHEN, A
CHEN, SJ
TONG, JH
WANG, ZY
WAXMAN, S
ZELENT, A
[J]. EMBO JOURNAL, 1993, 12 (03) : 1161 - 1167
[7] IDENTIFICATION AND NUCLEOTIDE-SEQUENCE OF A HUMAN LOCUS HOMOLOGOUS TO THE V-MYC ONCOGENE OF AVIAN MYELOCYTOMATOSIS VIRUS MC29
COLBY, WW
CHEN, EY
SMITH, DH
LEVINSON, AD
[J]. NATURE, 1983, 301 (5902) : 722 - 725
[8] COREY SJ, 1994, LEUKEMIA, V8, P1350
[9] GILLARD EF, 1993, SEMIN CANCER BIOL, V4, P359
[10] GRIGNANI F, 1994, BLOOD, V83, P10

← 1 2 3 →