1997
DOI: 10.1038/sj.onc.1201105
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K-ras modulates the cell cycle via both positive and negative regulatory pathways

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Cited by 66 publications
(39 citation statements)
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References 48 publications
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“…Since the phenotypes of RacV12 expression and E2F overexpression are similar, notably anchorage-independent growth and enhanced saturation density (5,7,40), we suggest that E2F stimulation contributes to the oncogenic potential of activated Rac. The ability of activated Rac and Cdc42 to up-regulate E2F transcriptional activity is consistent with published reports for the related small GTPase Ras, which, in its oncogenic form, also induces E2F-dependent transcription (41,42) (Fig. 1).…”
Section: Discussionsupporting
confidence: 90%
See 1 more Smart Citation
“…Since the phenotypes of RacV12 expression and E2F overexpression are similar, notably anchorage-independent growth and enhanced saturation density (5,7,40), we suggest that E2F stimulation contributes to the oncogenic potential of activated Rac. The ability of activated Rac and Cdc42 to up-regulate E2F transcriptional activity is consistent with published reports for the related small GTPase Ras, which, in its oncogenic form, also induces E2F-dependent transcription (41,42) (Fig. 1).…”
Section: Discussionsupporting
confidence: 90%
“…1). For Ras it is generally assumed that a significant contribution to its mitogenic potential comes from its ability to transcriptionally up-regulate cyclin D1 (34,35,41,(43)(44)(45). Ectopic expression of cyclin D1 accelerates G 1 progression (46), and it bypasses the need for Ras in proliferation of exponentially growing fibroblasts (47).…”
Section: Discussionmentioning
confidence: 99%
“…An activated K-RAS has been reported to modulate cycling cells through a wide spectrum of cell cycle regulators (30), but in particular, facilitates transition from G 2 -M into the next cycle (31). Our findings with Internavec were consistent with cell cycle blockage events that resulted from early viral gene expression as well as K-ras knockdown, culminating in S and G 2 -M phase arrests.…”
Section: Resultssupporting
confidence: 83%
“…24,25). These genes are associated with mitotic cell cycle, M phase, and cell proliferation, and the expression of some of them is reportedly controlled by Ras (25,26). Here, too, EXPANDER identified other genes that could represent novel putative NF-Y targets.…”
Section: Cancer Researchmentioning
confidence: 89%