IGF2 and cancer

Livingstone, Callum

doi:10.1530/erc-13-0231

Cited by 249 publications

(248 citation statements)

References 188 publications

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“…Parent-specific monoallelic expression increased vulnerability to cancer because loss of function of MEGs and reactivation of the silent maternal copy of PEGs would promote cellular proliferation and metastasis. Consistent with these predictions, expression of a cyclin-dependent kinase inhibitor CDKN1C (a MEG) is frequently reduced in cancer [74,75], whereas expression of an insulin-like growth factor IGF2 (a PEG) is frequently increased in cancer [76]. CDKN1C fits the initial predictions for a MEG closely, but not perfectly.…”

Section: Genomic Imprinting and The Subversion Of Intrinsic Defencesmentioning

confidence: 74%

Maternal–fetal conflict, genomic imprinting and mammalian vulnerabilities to cancer

Haig

2015

Phil. Trans. R. Soc. B

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Antagonistic coevolution between maternal and fetal genes, and between maternally and paternally derived genes may have increased mammalian vulnerability to cancer. Placental trophoblast has evolved to invade maternal tissues and evade structural and immunological constraints on its invasion. These adaptations can be co-opted by cancer in intrasomatic selection. Imprinted genes of maternal and paternal origin favour different degrees of proliferation of particular cell types in which they reside. As a result, the set of genes favouring greater proliferation will be selected to evade controls on cell-cycle progression imposed by the set of genes favouring lesser proliferation. The dynamics of stem cell populations will be a particular focus of this intragenomic conflict. Gene networks that are battlegrounds of intragenomic conflict are expected to be less robust than networks that evolve in the absence of conflict. By these processes, maternal–fetal and intragenomic conflicts may undermine evolved defences against cancer.

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Section: Genomic Imprinting and The Subversion Of Intrinsic Defencesmentioning

confidence: 74%

Maternal–fetal conflict, genomic imprinting and mammalian vulnerabilities to cancer

Haig

2015

Phil. Trans. R. Soc. B

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“…Similar challenges affecting knowledge of other human genes should promote attempts to critically evaluate, interpret, and correct human genetic data in publicly available databases. ________________________________________ Insulin-like growth factor 2 (IGF2 1 ), a conserved 67-amino acid, single-chain secreted protein, is intimately involved in several critical physiological processes in humans and other mammals (1)(2)(3)(4)(5)(6). IGF2, along with IGF1 and insulin, also comprises a gene family that is found in most mammalian species (7)(8)(9).…”

mentioning

confidence: 99%

The complex genetics of human insulin-like growth factor 2 are not reflected in public databases

Rotwein

2018

Journal of Biological Chemistry

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“…57 Insulin growth factor The IGF system is integral to a number of cellular processes ranging from normal growth and development of specific organs, such as in the nervous system, in which IGF signaling regulates neuronal proliferation, apoptosis, and cell survival. [58][59][60] Conversely, IGF also has a critical role in pathological situations, particularly tumorigenesis, and a growing body of epidemiological studies has implicated free IGF-1 serum levels as a risk factor for the development and progression of breast, prostate, colon, and lung cancer. 59,61,62 This adverse effect of IGF is unsurprising given the delicate balance that must be maintained, and the diverse and extensive regulatory function of IGF-1 in maintaining homeostasis.…”

Section: Growth Factor Driven Signaling In Tumor Metastasismentioning

confidence: 99%

The role of endocytic Rab GTPases in regulation of growth factor signaling and the migration and invasion of tumor cells

Porther

Barbieri

2015

Small GTPases

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Metastasis is characterized pathologically by uncontrolled cell invasion, proliferation, migration and angiogenesis. It is a multistep process that encompasses the modulation of membrane permeability and invasion, cell spreading, cell migration and proliferation of the extracellular matrix, increase in cell adhesion molecules and interaction, decrease in cell attachment and induced survival signals and propagation of nutrient supplies (blood vessels). In cancer, a solid tumor cannot expand and spread without a series of synchronized events. Changes in cell adhesion receptor molecules (e.g., integrins, cadherin-catenins) and protease expressions have been linked to tumor invasion and metastasis. It has also been determined that ligand-growth factor receptor interactions have been associated with cancer development and metastasis via the endocytic pathway. Specifically, growth factors, which include IGF-1 and IGF-2 therapy, have been associated with most if not all of the features of metastasis. In this review, we will revisit some of the key findings on perhaps one of the most important hallmarks of cancer metastasis: cell migration and cell invasion and the role of the endocytic pathway in mediating this phenomenon

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IGF2 and cancer

Cited by 249 publications

References 188 publications

Maternal–fetal conflict, genomic imprinting and mammalian vulnerabilities to cancer

Maternal–fetal conflict, genomic imprinting and mammalian vulnerabilities to cancer

The complex genetics of human insulin-like growth factor 2 are not reflected in public databases

The role of endocytic Rab GTPases in regulation of growth factor signaling and the migration and invasion of tumor cells

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