Binding of Ras to Phosphoinositide 3-Kinase p110α Is Required for Ras- Driven Tumorigenesis in Mice

Gupta, Surbhi; Ramjaun, Antoine R.; Haiko, Paula; Wang, Yihua; Warne, Patricia H.; Nicke, Barbara; Nye, Emma; Stamp, Gordon; Alitalo, Kari; Downward, Julian

doi:10.1016/j.cell.2007.03.051

Cited by 526 publications

(466 citation statements)

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“…recently been shown to be essential (Gupta et al, 2007). Here we characterize the nature of the requirement for Ras by showing that constitutively membrane-localized p110g and p110b do not require an interaction with Ras for full oncogenic activity.…”

Section: Discussionmentioning

confidence: 91%

Oncogenic signaling of class I PI3K isoforms

et al. 2007

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The catalytic subunits of class I PI3Ks comprise four isoforms: p110a, p110b, p110d and p110c. Cancer-specific gain-of-function mutations in p110a have been identified in various malignancies. Cancer-specific mutations in the non-a isoforms of class I PI3K have not yet been identified, however overexpression of either wild-type p110b, p110c or p110d is sufficient to induce cellular transformation in chicken embryo fibroblasts. The mechanism whereby these non-a isoforms of class I mediate oncogenic signals is unknown. Here we show that potently transforming class I isoforms signal via Akt/mTOR, inhibit GSK3b and cause degradation of FoxO1. A functional Erk pathway is required for p110c and p110b transformation but not for transformation by p110d or the H1047R mutant of p110a. Transformation and signaling by p110c and p110b are sensitive to loss of interaction with Ras, which acts as a membrane anchor. Mutations in the C2 domain of p110d reduce transformation, most likely by interfering with membrane association. Several small molecule inhibitors potently and specifically inhibit the oncogenic signaling and transformation of each of the class I PI3K, and, when used in combination with MEK inhibitors, can additively reduce the transformation induced by p110b and p110c.

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Section: Discussionmentioning

confidence: 91%

Oncogenic signaling of class I PI3K isoforms

et al. 2007

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“…Discs were stained for Fasciclin 3 to visualize disc outlines (blue) and for PH3 to mark cells in M-phase ((a-f) in red and (a 00 -e 00 ) and (f 0 ) in gray). PI3K signaling is low in Ras V12 , Dlg RNAi tumors From mammalian systems, it is known that Ras binds to PI3K and that oncogenic transformation in response to Ras depends on PI3K activity (Rodriguez-Viciana et al, 1994, 1997Gupta et al, 2007). In Drosophila, it was shown that PI3K is not required for physiological Ras signaling (Halfar et al, 2001;Prober and Edgar, 2002).…”

Section: Loss Of Pi3k Blocks Drosophila Tumor Growth M Willecke Et Almentioning

confidence: 99%

Loss of PI3K blocks cell-cycle progression in a Drosophila tumor model

2011

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Tumorigenesis is a complex process, which requires alterations in several tumor suppressor or oncogenes. Here, we use a Drosophila tumor model to identify genes, which are specifically required for tumor growth. We found that reduction of phosphoinositide 3-kinase (PI3K) activity resulted in very small tumors while only slightly affecting growth of wild-type tissue. The observed inhibition on tumor growth occurred at the level of cell-cycle progression. We conclude that tumor cells become dependent on PI3K function and that reduction of PI3K activity synthetically interferes with tumor growth. The results presented here broaden our insights into the intricate mechanisms underling tumorigenesis and illustrate the power of Drosophila genetics in revealing weak points of tumor progression.

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“…On the other hand, a recent studies using knock-in mice where the RBD of PI3K is substituted with a mutant RBD that is unable to bind Ras has shown that Ras-PI3K binding is essential for a variety of pathophysiological events, including the development of the lymphatic vasculature [42]. In endothelial cell lineages, the Ras-PI3K pathway and the internalization of vascular endothelial growth factor (VEGF) receptor 1 are involved in VEGF-dependent endothelial cell motility [43] and angiogenesis [44].…”

Section: /21mentioning

confidence: 99%

“…In endothelial cell lineages, the Ras-PI3K pathway and the internalization of vascular endothelial growth factor (VEGF) receptor 1 are involved in VEGF-dependent endothelial cell motility [43] and angiogenesis [44]. It is thus possible that a defect in the endocytosis of receptors such as VEGF receptor 3 in lymphatic endothelial cells is the cause of the impaired lymphatic development in PI3K mutant mice [42], considering the crucial role for Ras-PI3K signaling in local PIP 3 production in the endosome, as shown by this study (Fig. 5a-d and g).…”

Section: /21mentioning

confidence: 99%