THE TUMOR PROMOTER 12-O-TETRADECANOYLPHORBOL-13-ACETATE AND THE RAS ONCOGENE MODULATE EXPRESSION AND PHOSPHORYLATION OF GAP JUNCTION PROTEINS

被引：165

作者：

BRISSETTE, JL

KUMAR, NM

GILULA, NB

DOTTO, GP

机构：

[1] YALE UNIV, SCH MED, DEPT PATHOL, NEW HAVEN, CT 06510 USA

[2] Scripps Res Inst, RES INST, DEPT MOLEC BIOL, LA JOLLA, CA 92037 USA

来源：

MOLECULAR AND CELLULAR BIOLOGY | 1991年 / 11卷 / 10期

关键词：

D O I：

10.1128/MCB.11.10.5364

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：

Gap junctional intercellular communication is inhibited in response to tumor promoters and oncogene transformation, suggesting that loss of this function is an important step in tumor formation. To elucidate the molecular mechanisms responsible for this inhibition, we examined the expression of gap junction proteins and mRNA in mouse primary keratinocytes after treatment with the tumor promoter 12-O-tetradecanoylphorbol-13-acetate (TPA) and/or ras transformation. During normal cell growth, keratinocytes express the alpha-1 (connexin 43) and beta-2 (connexin 26) proteins. Within 5 min of TPA treatment, the alpha-1 protein became rapidly phosphorylated on serine residues and its expression was dramatically reduced by 24 h. The beta-2 protein, after an initial increase in expression, was also significantly reduced 24 h after treatment with TPA. ras transformation caused changes similar to those induced by TPA. The alpha-1 protein underwent an increase in serine phosphorylation, although its expression declined only slightly, while beta-2 expression was greatly reduced. The effects of TPA and ras on alpha-1 expression were additive; treatment of ras-transformed cells with TPA resulted in increased alpha-1 phosphorylation, with greatly decreased protein levels, much lower than those generated by either agent alone. These data provide a likely explanation for the similar and synergistic inhibition of gap junctional intercellular communication by phorbol esters and ras.

引用

页码：5364 / 5371

页数：8

共 60 条

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