INHIBITION OF PROLACTIN GENE-TRANSCRIPTION BY TRANSFORMING GROWTH-FACTOR-BETA IN GH3 CELLS

被引:48
作者
DELIDOW, BC [1 ]
BILLIS, WM [1 ]
AGARWAL, P [1 ]
WHITE, BA [1 ]
机构
[1] UNIV CONNECTICUT, CTR HLTH, DEPT ANAT, FARMINGTON, CT 06030 USA
来源
MOLECULAR ENDOCRINOLOGY | 1991年 / 5卷 / 11期
关键词
D O I
10.1210/mend-5-11-1716
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Transforming growth factor-beta (TGF-beta) is a member of a large family of growth factors, several of which regulate pituitary function. TGF-beta has recently been reported to reduce PRL production by GH4 cells. We have examined the effect of TGF-beta on PRL gene expression in rat pituitary tumor GH3 cells. TGF-beta-1 or TGF-beta-2 reduced both basal and Ca2+-stimulated PRL mRNA levels. This inhibition was specific, as the mRNA levels for GH, glucose-regulated protein 78, and histone-3 were unaffected by TGF-beta. Inhibition of PRL gene expression by TGF-beta was dose dependent in the range of 0.5-10 ng/ml. TGF-beta inhibited run-on PRL gene transcription in nuclei from treated cells to the same extent that it reduced PRL mRNA levels, indicating a transcriptional mechanism of action. However, TGF-beta did not affect Pit-1 mRNA levels or run-on transcription of the Pit-1 gene. Thus, TGF-beta does not appear to act through modification of Pit-1 gene expression. The PRL promotor contains two regions of homology, with a consensus sequence found in the promotors of other TGF-beta-inhibited genes. These findings are consistent with other studies that have demonstrated transcriptional repression by TGF-beta. The potency and specificity of the effects of TGF-beta on PRL gene expression suggest that it may be a physiological regulator of lactotroph function.
引用
收藏
页码:1716 / 1722
页数:7
相关论文
共 49 条
[31]   EPIDERMAL GROWTH-FACTOR RAPIDLY STIMULATES PROLACTIN GENE-TRANSCRIPTION [J].
MURDOCH, GH ;
POTTER, E ;
NICOLAISEN, AK ;
EVANS, RM ;
ROSENFELD, MG .
NATURE, 1982, 300 (5888) :192-194
[32]   A TRANSCRIPT FROM A DROSOPHILA PATTERN GENE PREDICTS A PROTEIN HOMOLOGOUS TO THE TRANSFORMING GROWTH-FACTOR-BETA FAMILY [J].
PADGETT, RW ;
STJOHNSTON, RD ;
GELBART, WM .
NATURE, 1987, 325 (6099) :81-84
[33]   CHARACTERIZATION OF A CDNA CLONE ENCODING MURINE MITOGEN-REGULATED PROTEIN - REGULATION OF MESSENGER-RNA LEVELS IN MORTAL AND IMMORTAL CELL-LINES [J].
PARFETT, CLJ ;
HAMILTON, RT ;
HOWELL, BW ;
EDWARDS, DR ;
NILSENHAMILTON, M ;
DENHARDT, DT .
MOLECULAR AND CELLULAR BIOLOGY, 1985, 5 (11) :3289-3292
[34]   THYROTROPIN-RELEASING-HORMONE EXERTS RAPID NUCLEAR EFFECTS TO INCREASE PRODUCTION OF THE PRIMARY PROLACTIN MESSENGER-RNA TRANSCRIPT [J].
POTTER, E ;
NICOLAISEN, AK ;
ONG, ES ;
EVANS, RM ;
ROSENFELD, MG .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1981, 78 (11) :6662-6666
[35]   TRANSCRIPTIONAL AND POSTTRANSCRIPTIONAL REGULATION OF THE RAT PROLACTIN GENE BY CALCIUM [J].
PRESTON, GM ;
BILLIS, WM ;
WHITE, BA .
MOLECULAR AND CELLULAR BIOLOGY, 1990, 10 (02) :442-448
[36]   TRANSFORMING GROWTH FACTOR-ALPHA AND FACTOR-BETA ARE POTENT AND EFFECTIVE INHIBITORS OF GH4 PITUITARY-TUMOR CELL-PROLIFERATION [J].
RAMSDELL, JS .
ENDOCRINOLOGY, 1991, 128 (04) :1981-1990
[37]   A NEW CLONAL STRAIN OF RAT PITUITARY-TUMOR CELLS - A MODEL FOR NON-REGULATED SECRETION OF PROLACTIN [J].
REYMOND, MJ ;
NANSEL, DD ;
BURROWS, GH ;
NEAVES, WB ;
PORTER, JC .
ACTA ENDOCRINOLOGICA, 1984, 106 (04) :459-470
[38]   MESODERM INDUCTION IN AMPHIBIANS - THE ROLE OF TGF-BETA-2-LIKE FACTORS [J].
ROSA, F ;
ROBERTS, AB ;
DANIELPOUR, D ;
DART, LL ;
SPORN, MB ;
DAWID, IB .
SCIENCE, 1988, 239 (4841) :783-785
[39]   HORMONE-MEDIATED REPRESSION - A NEGATIVE GLUCOCORTICOID RESPONSE ELEMENT FROM THE BOVINE PROLACTIN GENE [J].
SAKAI, DD ;
HELMS, S ;
CARLSTEDTDUKE, J ;
GUSTAFSSON, JA ;
ROTTMAN, FM ;
YAMAMOTO, KR .
GENES & DEVELOPMENT, 1988, 2 (09) :1144-1154
[40]   MEASUREMENT OF PEPTIDE SECRETION AND GENE-EXPRESSION IN THE SAME CELL [J].
SCARBROUGH, K ;
WEILAND, NG ;
LARSON, GH ;
SORTINO, MA ;
CHIU, S ;
HIRSHFIELD, AN ;
WISE, PM .
MOLECULAR ENDOCRINOLOGY, 1991, 5 (01) :134-142
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