RETINOIC ACID POSTTRANSCRIPTIONALLY UP-REGULATES PROTEOLIPID PROTEIN GENE-EXPRESSION IN C6 GLIOMA-CELLS

被引:0
|
作者
LOPEZBARAHONA, M
MINANO, M
MIRA, E
IGLESIAS, T
STUNNENBERG, HG
RODRIGUEZPENA, A
BERNAL, J
MUNOZ, A
机构
[1] CSIC,INST INVEST BIOMED,ARTURO DUPERIER 4,E-28029 MADRID,SPAIN
[2] ANTIBIOT FARMA SA,DEPT INVEST,E-28026 MADRID,SPAIN
[3] EUROPEAN MOLEC BIOL LAB,W-6900 HEIDELBERG,GERMANY
来源
JOURNAL OF BIOLOGICAL CHEMISTRY | 1993年 / 268卷 / 34期
关键词
D O I
暂无
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The proteolipid protein (PLP) gene codes for the major central nervous system myelin protein. We have studied the effects of different agents on the expression of the PLP gene in C6 glioma cells. Retinoic acid (RA), but not dexamethasone, estradiol, insulin, growth hormone, or vitamin D3, had a drastic effect, increasing 10-20-fold the level of PLP mRNA. Concomitantly, RA also induced the appearance of the corresponding immunoreactive protein. The increase in PLP RNA level showed a slow kinetics and was blocked by cycloheximide, suggesting a posttranscriptional regulation by RA. Nuclear run-on assays confirmed that the rate of PLP gene transcription was unchanged by RA. In contrast, we found that retinoic acid augmented PLP mRNA stability, causing a substantial increase in its half-life. RA action was independent of cell density, serum, or PDGF but was partially inhibited by bFGF. On the other hand, thyroid hormone caused a moderate increase in PLP mRNA levels in C6 cells but only when the low numbers of thyroid receptors in these cells were increased by retrovirally mediated expression of an exogenous c-erbA/TRalpha-1 gene. Our results indicate that RA specifically up-regulates PLP expression in glioma C6 cells at a posttranscriptional level by increasing PLP RNA half-life.
引用
收藏
页码:25617 / 25623
页数:7
相关论文
共 50 条
  • [21] INTERACTIONS OF C6 GLIOMA-CELLS WITH LAMININ AND FIBRONECTIN
    PALM, SL
    FURCHT, LT
    JOURNAL OF CELL BIOLOGY, 1986, 103 (05): : A95 - A95
  • [22] ENHANCEMENT OF RADIOSENSITIVITY BY TAMOXIFEN IN C6 GLIOMA-CELLS
    WEI, Z
    YAMADA, H
    SAKAI, N
    NIIKAWA, S
    NOZAWA, Y
    OLSON, J
    VERTOSICK, FT
    NEUROSURGERY, 1992, 31 (04) : 725 - 730
  • [23] NEURONOTROPHIC FACTORS RELEASED BY C6 GLIOMA-CELLS
    WESTERMANN, R
    HARDUNG, M
    MEYER, DK
    EHRHARD, P
    OTTEN, U
    UNSICKER, K
    JOURNAL OF NEUROCHEMISTRY, 1988, 50 (06) : 1747 - 1758
  • [24] INVADING C6 GLIOMA-CELLS MAINTAINING TUMORIGENICITY
    CHICOINE, MR
    SILBERGELD, DL
    JOURNAL OF NEUROSURGERY, 1995, 83 (04) : 665 - 671
  • [25] REGULATION OF CONNEXIN43 EXPRESSION IN C6 GLIOMA-CELLS BY FORSKOLIN
    BECHBERGER, JF
    DEAKIN, M
    CAVENEY, S
    NAUS, CCG
    MOLECULAR BIOLOGY OF THE CELL, 1992, 3 : A294 - A294
  • [26] PROTEIN DEPHOSPHORYLATION IS NECESSARY FOR VOLUME REGULATORY DECREASE IN C6 GLIOMA-CELLS
    LOHR, JW
    CLINICAL RESEARCH, 1992, 40 (02): : A181 - A181
  • [27] EFFECTS OF TRIFLUOROACETIC-ACID, A HALOTHANE METABOLITE, ON C6 GLIOMA-CELLS
    MA, TG
    LING, YH
    MCCLURE, GD
    TSENG, MT
    JOURNAL OF TOXICOLOGY AND ENVIRONMENTAL HEALTH, 1990, 31 (02): : 147 - 158
  • [28] PROTEIN-GROWTH FACTOR(S) FROM C6 GLIOMA-CELLS
    SHARMA, SK
    JOURNAL OF IMMUNOLOGICAL METHODS, 1992, 154 (02) : 269 - 270
  • [29] EFFECT OF CULTURE CONDITIONS ON PLP AND MAG GENE-EXPRESSION IN RAT GLIOMA C6 CELLS
    KANOH, M
    YE, P
    ZHU, W
    WIGGINS, RC
    KONAT, G
    METABOLIC BRAIN DISEASE, 1991, 6 (03) : 133 - 143
  • [30] PROENKEPHALIN GENE-EXPRESSION IN C6 RAT GLIOMA-CELLS - POTENTIATION OF CYCLIC ADENOSINE 3',5'-MONOPHOSPHATE-DEPENDENT TRANSCRIPTION BY GLUCOCORTICOIDS
    JOSHI, J
    SABOL, SL
    MOLECULAR ENDOCRINOLOGY, 1991, 5 (08) : 1069 - 1080
12345