Alternative RNA splicing of the MLL gene in normal and malignant cells

被引：26

作者：

Nam, DK ^{[1
]}

Honoki, K ^{[1
]}

Yu, M ^{[1
]}

Yunis, JJ ^{[1
]}

机构：

[1] THOMAS JEFFERSON UNIV,JEFFERSON MED COLL,DEPT PATHOL ANAT & CELL BIOL,DIV CANC BIOL,PHILADELPHIA,PA 19107

来源：

GENE | 1996年 / 178卷 / 1-2期

关键词：

alternative RNA splicing; MLL protein motifs; homeobox genes; hematopoietic cells; leukemia; RT-PCR; cloning; DNA sequencing; northern blot;

D O I：

10.1016/0378-1119(96)00364-2

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The human MLL(mixed-lineage leukemia or myeloid-lymphoid leukemia) gene belongs to the trithorax gene family of which the Drosophila trithorax (trx) gene is known to regulate homeotic genes through alternative RNA splicing. To test if such a splicing mechanism also operates in MLL, we evaluated mRNA transcripts from a large number of normal and malignant human cells, making use of RT-PCR, PCR cloning, DNA sequencing and Northern blot analysis. Our findings indicate that different cell types transcribe MLL mRNA species lacking exons that generally encode putative regulatory domains such as AT hooks (exon 3), repression domain (exon 6), zinc finger motifs (exon 8) and activation domain (exon 18). Such findings suggest that posttranscriptional regulation by alternative RNA splicing may play an important role in MLL gene expression and provides the rationale for a mechanism by which this gene, with multiple functional domains, could produce discrete protein products that may prove critical in the regulation of human homeobox genes.

引用

页码：169 / 175

页数：7

共 38 条

[1]

BASERGA S, 1988, P NATL ACAD SCI USA, V85, P2956

[2] MODULATION OF DNA-BINDING SPECIFICITY BY ALTERNATIVE SPLICING OF THE WILMS-TUMOR WT1 GENE TRANSCRIPT [J].

BICKMORE, WA ;

OGHENE, K ;

LITTLE, MH ;

SEAWRIGHT, A ;

VANHEYNINGEN, V ;

HASTIE, ND .

SCIENCE, 1992, 257 (5067) :235-237

[3]

BOMZE HM, 1994, GENETICS, V136, P965

[4]

BREEN TR, 1993, DEVELOPMENT, V117, P119

[5] MULTIPLE CLOSELY-LINKED NFAT-OCTAMER AND HMG I(Y) BINDING-SITES ARE PART OF THE INTERLEUKIN-4 PROMOTER [J].

CHUVPILO, S ;

SCHOMBERG, C ;

GERWIG, R ;

HEINFLING, A ;

REEVES, R ;

GRUMMT, F ;

SERFLING, E .

NUCLEIC ACIDS RESEARCH, 1993, 21 (24) :5694-5704

[6]

CIMINO G, 1991, CANCER RES, V51, P6712

[7]

CLAUS P, 1994, J BIOL CHEM, V269, P33042

[8] ACUTE LEUKEMIAS OF DIFFERENT LINEAGES HAVE SIMILAR MLL GENE FUSIONS ENCODING RELATED CHIMERIC PROTEINS RESULTING FROM CHROMOSOMAL TRANSLOCATION [J].

CORRAL, J ;

FORSTER, A ;

THOMPSON, S ;

LAMPERT, F ;

KANEKO, Y ;

SLATER, R ;

KROES, WG ;

VANDERSCHOOT, CE ;

LUDWIG, WD ;

KARPAS, A ;

POCOCK, C ;

COTTER, F ;

RABBITTS, TH .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (18) :8538-8542

[9] A COMPREHENSIVE SET OF SEQUENCE-ANALYSIS PROGRAMS FOR THE VAX [J].

DEVEREUX, J ;

HAEBERLI, P ;

SMITHIES, O .

NUCLEIC ACIDS RESEARCH, 1984, 12 (01) :387-395

[10] A TRITHORAX-LIKE GENE IS INTERRUPTED BY CHROMOSOME 11Q23 TRANSLOCATIONS IN ACUTE LEUKEMIAS [J].

DJABALI, M ;

SELLERI, L ;

PARRY, P ;

BOWER, M ;

YOUNG, BD ;

EVANS, GA .

NATURE GENETICS, 1992, 2 (02) :113-118

← 1 2 3 4 →