The Ras-ERK and PI3K-mTOR pathways: cross-talk and compensation

Mendoza, Michelle C.; Er, Ekrem Emrah; Blenis, John

doi:10.1016/j.tibs.2011.03.006

Cited by 1,445 publications

(1,314 citation statements)

References 99 publications

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“…The ERK1/2 signaling pathway has the ability to regulate proteins involved in the initiation and elongation stages of mRNA translation in an mTOR-dependent and -independent manner (28,35,43,44). Recent studies indicated that ERK signaling is involved in later phase anabolic responses after resistance exercise (5,6,15).…”

Section: Discussionmentioning

confidence: 99%

mTOR signaling response to resistance exercise is altered by chronic resistance training and detraining in skeletal muscle

Ogasawara

Kobayashi

Tsutaki

et al. 2013

Journal of Applied Physiology

116

101

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Section: Discussionmentioning

confidence: 99%

mTOR signaling response to resistance exercise is altered by chronic resistance training and detraining in skeletal muscle

Ogasawara

Kobayashi

Tsutaki

et al. 2013

Journal of Applied Physiology

116

101

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show abstract

“…8,9 In addition, Ras proteins can also activate PI3K, mediating proliferative and survival signals. 10,11 The GAP domain of DAB2IP is homologous to other RasGAPs, such as GAP120 and neurofibromin (NF1), and can stimulate the GTPase activity of RAS proteins both in vitro and in cancer cell lines (Figure 2). [12][13][14][15] In prostate cancer cells, DAB2IP was shown to be recruited by the adaptor protein DAB2/DOC2 to promote Ras inactivation and inhibition of MAPK signaling upon receptor stimulation.…”

Section: Dab2ip: a Complex Gene Encoding A Negative Modulator Of Multmentioning

confidence: 99%

“…The GAP activity of DAB2IP can further enforce inhibition of the PI3K-AKT axis by reducing Ras-dependent activation of PI3K p110α subunit. 10,11 Interestingly, animal models showed that DAB2IP functions as endogenous inhibitor of adaptive angiogenesis in part by binding directly to VEGFR-2 and limiting PI3K activation ( Figure 4b). 4 GSK3β-β-catenin signaling.…”

Section: Dab2ip: a Complex Gene Encoding A Negative Modulator Of Multmentioning

confidence: 99%

Block one, unleash a hundred. Mechanisms of DAB2IP inactivation in cancer

2016

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One of the most defining features of cancer is aberrant cell communication; therefore, a molecular understanding of the intricate network established among tumor cells and their microenvironment could significantly improve comprehension and clinical management of cancer. The tumor suppressor DAB2IP (Disabled homolog 2 interacting protein), also known as AIP1 (ASK1 interacting protein), has an important role in this context, as it modulates signal transduction by multiple inflammatory cytokines and growth factors. DAB2IP is a Ras-GAP, and negatively controls Ras-dependent mitogenic signals. In addition, acting as a signaling adaptor, DAB2IP modulates other key oncogenic pathways, including TNFα/NF-κB, WNT/β-catenin, PI3K/AKT, and androgen receptors. Therefore, DAB2IP inactivation can provide a selective advantage to tumors initiated by a variety of driver mutations. In line with this role, DAB2IP expression is frequently impaired by methylation in cancer. Interestingly, recent studies reveal that tumor cells can employ other sophisticated mechanisms to disable DAB2IP at the post-transcriptional level. We review the mechanisms and consequences of DAB2IP inactivation in cancer, with the purpose to support and improve research aimed to counteract such mechanisms. We suggest that DAB2IP reactivation in cancer cells could be a strategy to coordinately dampen multiple oncogenic pathways, potentially limiting progression of a wide spectrum of tumors.

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“…Important signal-transduction pathways linking regulation of protein synthesis to nutrient sensing are mitogen-activated protein kinase and target of rapamycin signalling cascades. However, as the connection of these signalling pathways to translational regulation and cell growth has been extensively reviewed, they will not be further discussed here (for more information see reviews [11][12][13][14]). …”

Section: Introductionmentioning

confidence: 99%

Translational regulation of the cell cycle: when, where, how and why?

Kronja

Orr‐Weaver

2011

Phil. Trans. R. Soc. B

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Translational regulation contributes to the control of archetypal and specialized cell cycles, such as the meiotic and early embryonic cycles. Late meiosis and early embryogenesis unfold in the absence of transcription, so they particularly rely on translational repression and activation of stored maternal mRNAs. Here, we present examples of cell cycle regulators that are translationally controlled during different cell cycle and developmental transitions in model organisms ranging from yeast to mouse. Our focus also is on the RNA-binding proteins that affect cell cycle progression by recognizing special features in untranslated regions of mRNAs. Recent research highlights the significance of the cytoplasmic polyadenylation element-binding protein (CPEB). CPEB determines polyadenylation status, and consequently translational efficiency, of its target mRNAs in both transcriptionally active somatic cells as well as in transcriptionally silent mature Xenopus oocytes and early embryos. We discuss the role of CPEB in mediating the translational timing and in some cases spindle-localized translation of critical regulators of Xenopus oogenesis and early embryogenesis. We conclude by outlining potential directions and approaches that may provide further insights into the translational control of the cell cycle.

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The Ras-ERK and PI3K-mTOR pathways: cross-talk and compensation

Cited by 1,445 publications

References 99 publications

mTOR signaling response to resistance exercise is altered by chronic resistance training and detraining in skeletal muscle

mTOR signaling response to resistance exercise is altered by chronic resistance training and detraining in skeletal muscle

Block one, unleash a hundred. Mechanisms of DAB2IP inactivation in cancer

Translational regulation of the cell cycle: when, where, how and why?

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