INDUCTION OF RET PROTOONCOGENE EXPRESSION IN NEUROBLASTOMA-CELLS PRECEDES NEURONAL DIFFERENTIATION AND IS NOT MEDIATED BY PROTEIN-SYNTHESIS

被引：52

作者：

BUNONE, G

BORRELLO, MG

PICETTI, R

BONGARZONE, I

PEVERALI, FA

DEFRANCISCIS, V

DELLAVALLE, G

PIEROTTI, MA

机构：

[1] UNIV PAVIA,DIPARTIMENTO GENET & MICROBIOL,I-27100 PAVIA,ITALY

[2] IST NAZL TUMORI,DIV ONCOL SPERIMENTALE A,I-20133 MILAN,ITALY

[3] UNIV NAPLES,DIPARTIMENTO BIOL & PATOL CELLULARE,NAPLES,ITALY

来源：

EXPERIMENTAL CELL RESEARCH | 1995年 / 217卷 / 01期

关键词：

D O I：

10.1006/excr.1995.1067

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

RET proto-oncogene products are involved in neural crest development, and constitutional RET mutations are associated with syndromes characterized by tumors of neural crest origin. To study the regulation of RET transcription during neuronal differentiation we analyzed RET expression in neuroblastoma cell lines treated with various differentiating agents. A marked increase in RET mRNA levels was observed in all the cell lines examined shortly after retinoic acid (RA) treatment and before the onset of detectable morphological changes. Upregulation of RET expression was also found in SK-N-BE cells induced to differentiate by 12-O-tetradecanoylphorbol-13-acetate, glial cell-conditioned medium, alpha or gamma interferon, and in SH-SY-5Y cells exposed to nerve growth factor. Induction of RET expression by RA occurred in the absence of de novo protein synthesis. On the other hand, cycloheximide treatment by itself caused upregulation of RET transcripts. These results indicate that the positive transcriptional regulation of RET is closely associated with early neuronal differentiation and suggest that a negative regulatory factor/s controls RET transcription in neuroblastoma cells. Finally, anti-Ret antibodies immunoprecipitated four bands with apparent molecular weights of 150, 155, 170, and 175 kDa in RA-induced SK-N-BE cells. These bands likely represent differently glycosylated forms of the two RET primary products (117 and 122 kDa) detected in tunicamycin-treated cells. (C) 1995 Academic Press, Inc.

引用

页码：92 / 99

页数：8

共 44 条

[1] AVANTAGGIATO V, 1994, CELL GROWTH DIFFER, V5, P305
[2] BIEDLER JL, 1978, CANCER RES, V38, P3751
[3] BONGARZONE I, 1989, ONCOGENE, V4, P1457
[4] MOLECULAR CHARACTERIZATION OF A THYROID TUMOR-SPECIFIC TRANSFORMING SEQUENCE FORMED BY THE FUSION OF RET TYROSINE KINASE AND THE REGULATORY SUBUNIT RI-ALPHA OF CYCLIC AMP-DEPENDENT PROTEIN KINASE-A
BONGARZONE, I
MONZINI, N
BORRELLO, MG
CARCANO, C
FERRARESI, G
ARIGHI, E
MONDELLINI, P
DELLAPORTA, G
PIEROTTI, MA
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1993, 13 (01) : 358 - 366
[5] TRK AND RET PROTOONCOGENE EXPRESSION IN HUMAN NEUROBLASTOMA SPECIMENS - HIGH-FREQUENCY OF TRK EXPRESSION IN NON-ADVANCED STAGES
BORRELLO, MG
BONGARZONE, I
PIEROTTI, MA
LUKSCH, R
GASPARINI, M
COLLINI, P
PILOTTI, S
RIZZETTI, MG
MONDELLINI, P
DEBERNARDI, B
DIMARTINO, D
GARAVENTA, A
BRISIGOTTI, M
TONINI, GP
[J]. INTERNATIONAL JOURNAL OF CANCER, 1993, 54 (04) : 540 - 545
[6] CHOMCZYNSKI P, 1986, ANAL BIOCHEM, V162, P156
[7] CHARACTERIZATION OF A RETINOIC ACID RESPONSIVE ELEMENT ISOLATED BY WHOLE GENOME PCR
COSTAGIOMI, MP
GAUB, MP
CHAMBON, P
ABARZUA, P
[J]. NUCLEIC ACIDS RESEARCH, 1992, 20 (12) : 3223 - 3232
[8] MUTATIONS IN THE RET PROTOONCOGENE ARE ASSOCIATED WITH MEN 2A AND FMTC
DONISKELLER, H
DOU, SS
CHI, D
CARLSON, KM
TOSHIMA, K
LAIRMORE, TC
HOWE, JR
MOLEY, JF
GOODFELLOW, P
WELLS, SA
[J]. HUMAN MOLECULAR GENETICS, 1993, 2 (07) : 851 - 856
[9] MUTATIONS OF THE RET PROTOONCOGENE IN HIRSCHSPRUNGS-DISEASE
EDERY, P
LYONNET, S
MULLIGAN, LM
PELET, A
DOW, E
ABEL, L
HOLDER, S
NIHOULFEKETE, C
PONDER, BAJ
MUNNICH, A
[J]. NATURE, 1994, 367 (6461) : 378 - 380
[10] DO INFANTS WITH STAGE IV-S NEURO-BLASTOMA NEED TREATMENT
EVANS, AE
BAUM, E
CHARD, R
[J]. ARCHIVES OF DISEASE IN CHILDHOOD, 1981, 56 (04) : 271 - 274

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