A role for Sam68 in cell cycle progression antagonized by a spliced variant within the KH domain

被引：84

作者：

Barlat, I ^{[1
]}

Maurier, F ^{[1
]}

Duchesne, M ^{[1
]}

Guitard, E ^{[1
]}

Tocque, B ^{[1
]}

Schweighoffer, F ^{[1
]}

机构：

[1] RHONE POULENC RORER,GENE MED DEPT,F-94403 VITRY SUR SEINE,FRANCE

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1997年 / 272卷 / 06期

关键词：

D O I：

10.1074/jbc.272.6.3129

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：

Sam68 is the main tyrosine-phosphorylated and Src-associated protein in mitotic cells. Sam68 exhibits a conserved functional KH (hnRNPK homology) RNA binding domain and binds single strand nucleic acids. Tyrosine phosphorylation mediates the interaction of Sam68 with many SH3- and SH2-containing proteins and negatively regulates its nucleic acid binding properties. But the function and the impact of Sam68 on cell signaling and cell proliferation remains elusive. We report here the identification of a natural isoform of Sam68 with a deletion within the KH domain. This isoform, called Sam68 Delta KH, is specifically expressed at growth arrest upon confluency in normal cells. In cells that do not enter quiescence at confluency such as Src-transformed cells, no recruitment of Sam68 Delta KH is observed. Transfected Sam68 Delta KH inhibits serum-induced DNA synthesis and cyclin D1 expression. Sam68 overcomes these effects, suggesting that isoforms of Sam68 are involved, through KH domain signaling, in cell proliferation, and more precisely in G(1)/S transition.

引用

页码：3129 / 3132

页数：4

共 22 条

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