The Insulin-Like Growth Factor-I Receptor

Meyts, Pierre De; Wallach, Brenda; Christoffersen, Claus T.; Ursø, Birgitte; Grønskov, Karen; Latus, Lori-Jo; Yakushiji, Fumiatsu; Ilondo, M M; Shymko, Ronald M.

doi:10.1159/000184188

Cited by 218 publications

(66 citation statements)

References 79 publications

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“…Shc expression is equal among all the neuroblastoma cell lines tested (Figure 2d). Two of the major downstream signaling pathways that mediate (De Meyts et al, 1994;Cheatham and Kahn, 1995;Miller et al, 1997;Kim and Feldman, 1998;Kim et al, 1998a). All the neuroblastoma cell lines we tested express similar levels of Akt and p42/p44 MAPK (Figure 2e and f).…”

Section: Expression Of Signaling Molecules In the Neuroblastoma Cell mentioning

confidence: 88%

“…Upon ligand binding of the IGF-IR, autophosphorylation of its b-subunits occurs, resulting in binding of the major IGF-IR substrates, insulin receptor substrate (IRS)-1, -2 and Shc (Pronk et al, 1993;Giorgetti et al, 1994;Myers and White, 1996). The signaling pathways mediated by Shc and IRS proteins, including the mitogen-activated protein kinase (MAPK) and phosphatidylinositol-3 kinase (PI 3-K) pathways, are implicated in the effects of IGF-I on cell survival, mitogenesis, differentiation and cytoskeletal changes (De Meyts et al, 1994;Cheatham and Kahn, 1995;Miller et al, 1997;Kim and Feldman, 1998;Kim et al, 1998a). Targeted disruption of IGF-IR signaling by antisense mRNA or dominant-negative mutants results in inhibition of tumorigenesis in vivo and in vitro by allowing apoptosis to occur (Liu et al, 1998;Reiss et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

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Insulin-like growth factor-I signaling in human neuroblastoma cells

2004

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Section: Expression Of Signaling Molecules In the Neuroblastoma Cell mentioning

confidence: 88%

Section: Introductionmentioning

confidence: 99%

Insulin-like growth factor-I signaling in human neuroblastoma cells

2004

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“…For example, insulin, acting through its receptor, triggers a number of biological responses which can be divided into two broad categories. Metabolic processes, associated with uptake and subsequent storage of glucose, are generally taken to be the primary target of insulin receptor signalling, but mitogenic processes associated with DNA replication, cell growth and division are also activated to a lesser or greater degree (for reviews, see [1][2][3]). Both kinds of signalling begin with hormone binding, which results in receptor autophosphorylation and activation of the receptor tyrosine kinase, followed by a cascade of activation of intracellular signalling molecules (Scheme 1) [4,5].…”

Section: Introductionmentioning

confidence: 99%

Logical analysis of timing-dependent receptor signalling specificity: application to the insulin receptor metabolic and mitogenic signalling pathways

Shymko¹,

Meyts²,

Thomas

1997

Biochemical Journal

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We present a method for logical analysis of signal-transduction networks, focusing on metabolic and mitogenic signalling by the insulin receptor, with specific emphasis on dependence of the signalling properties on the timing of binding events. We discuss a basic model which demonstrates this dependence (hormone binding leads to activation of the receptor which can lead to a commitment to mitogenic signalling), and show how residence time of the hormone on the receptor can determine the specificity

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“…However, both insulin and IGF-1 can induce mitogenic and metabolic effects in normal cells. It is unclear whether each ligand elicits these activities via its own receptor, or whether insulin exerts its mitogenic effects through its weak affinity binding to the IGF-1 receptor, and IGF-1 exerts its metabolic effects through the insulin receptor (3,4).…”

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confidence: 99%

Peptides Identify the Critical Hotspots Involved in the Biological Activation of the Insulin Receptor

Pillutla¹,

Hsiao²,

Beasley³

et al. 2002

Journal of Biological Chemistry

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We used phage display to generate surrogate peptides that define the hotspots involved in protein-protein interaction between insulin and the insulin receptor. All of the peptides competed for insulin binding and had affinity constants in the high nanomolar to low micromolar range. Based on competition studies, peptides were grouped into non-overlapping Sites 1, 2, or 3. Some Site 1 peptides were able to activate the tyrosine kinase activity of the insulin receptor and act as agonists in the insulin-dependent fat cell assay, suggesting that Site 1 marks the hotspot involved in insulin-induced activation of the insulin receptor. On the other hand, Site 2 and 3 peptides were found to act as antagonists in the phosphorylation and fat cell assays. These data show that a peptide display can be used to define the molecular architecture of a receptor and to identify the critical regions required for biological activity in a site-directed manner.

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The Insulin-Like Growth Factor-I Receptor

Cited by 218 publications

References 79 publications

Insulin-like growth factor-I signaling in human neuroblastoma cells

Insulin-like growth factor-I signaling in human neuroblastoma cells

Logical analysis of timing-dependent receptor signalling specificity: application to the insulin receptor metabolic and mitogenic signalling pathways

Peptides Identify the Critical Hotspots Involved in the Biological Activation of the Insulin Receptor

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