FUNCTIONAL INTERACTION BETWEEN E2F-4 AND P130 - EVIDENCE FOR DISTINCT MECHANISMS UNDERLYING GROWTH SUPPRESSION BY DIFFERENT RETINOBLASTOMA PROTEIN FAMILY MEMBERS

被引：299

作者：

VAIRO, G

LIVINGSTON, DM

GINSBERG, D

机构：

[1] DANA FARBER CANC INST,BOSTON,MA 02115

[2] HARVARD UNIV,SCH MED,BOSTON,MA 02115

来源：

GENES & DEVELOPMENT | 1995年 / 9卷 / 07期

关键词：

E2F; CELL CYCLE; TRANSCRIPTION FACTOR; G(0); P130; RB FAMILY;

D O I：

10.1101/gad.9.7.869

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Little is known of the mechanisms controlling the G(0)/G(1) transition of the cell cycle. The induction of immediate early gene expression, thought to be important for this process, suggests that the key factors controlling this transition preexist in quiescent cells. The E2F family of transcription factors likely play an important role in this process, because E2F DNA-binding activity exists in quiescent cells, and the induction of at least some immediate early genes requires intact E2F regulatory promoter sites. Here, we show that the major G(0) E2F activity of primary human T cells, E2F-4, is stably bound to the p130 pocket protein in association with a DP heterodimerization partner. p130-E2F-4 binding has functional implications because p130 effectively suppressed E2F-4-mediated trans-activation, and coexpression of E2F-4 overcame p130-mediated G(1) arrest more efficiently than RB-induced G(1) blockade. Conversely, E2F-1 overrode an RB-induced G(1) block more efficiently than E2F-4. Thus, p130 and RB appear to induce cell cycle arrest via biochemically distinct mechanisms that involve different E2F family members.

引用

页码：869 / 881

页数：13

共 62 条

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