Interaction of Insulin-like Growth Factor II (IGF-II) with Multiple Plasma Proteins

Oesterreicher, Sandra; Blum, Werner; Schmidt, Bernhard; Braulke, Thomas; Kübler, Bernd

doi:10.1074/jbc.m411754200

Cited by 17 publications

(5 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The IGFBPs 1-7 and 9. Insulin-like growth factor-II has been shown to bind to most of the soluble extracellular proteins of the IGFBP family, as reviewed elsewhere [49][50][51]. The cumulative effect of IGF-II binding proteins towards the IGF-II levels in the bloodstream might mitigate its increased exposure to local tissues.…”

Section: The Igf-ii Binders: a Fine-tuned System For The Control Of Imentioning

confidence: 99%

“…Transferrin (TF). TF has been shown to be a constitutive component of the 150kDa trimeric IGF binding protein complex found in the bloodstream [51]. Its binding to IGFs (I and II) is less strong than other IGF-IGFBP interactions (where the highest affinity is shown with IGFBP3), and its physiological role is still to be determined.…”

Section: The Igf-ii Binders: a Fine-tuned System For The Control Of Imentioning

confidence: 99%

See 1 more Smart Citation

The IGF-II–Insulin Receptor Isoform-A Autocrine Signal in Cancer: Actionable Perspectives

Scalia

Giordano

2020

Cancers

View full text Add to dashboard Cite

Insulin receptor overexpression is a common event in human cancer. Its overexpression is associated with a relative increase in the expression of its isoform A (IRA), a shorter variant lacking 11 aa in the extracellular domain, conferring high affinity for the binding of IGF-II along with added intracellular signaling specificity for this ligand. Since IGF-II is secreted by the vast majority of malignant solid cancers, where it establishes autocrine stimuli, the co-expression of IGF-II and IRA in cancer provides specific advantages such as apoptosis escape, growth, and proliferation to those cancers bearing such a co-expression pattern. However, little is known about the exact role of this autocrine ligand–receptor system in sustaining cancer malignant features such as angiogenesis, invasion, and metastasis. The recent finding that the overexpression of angiogenic receptor kinase EphB4 along with VEGF-A is tightly dependent on the IGF-II/IRA autocrine system independently of IGFIR provided new perspectives for all malignant IGF2omas (those aggressive solid cancers secreting IGF-II). The present review provides an updated view of the IGF system in cancer, focusing on the biology of the autocrine IGF-II/IRA ligand–receptor axis and supporting its underscored role as a malignant-switch checkpoint target.

show abstract

Section: The Igf-ii Binders: a Fine-tuned System For The Control Of Imentioning

confidence: 99%

Section: The Igf-ii Binders: a Fine-tuned System For The Control Of Imentioning

confidence: 99%

The IGF-II–Insulin Receptor Isoform-A Autocrine Signal in Cancer: Actionable Perspectives

Scalia

Giordano

2020

Cancers

View full text Add to dashboard Cite

show abstract

“…No specific cell surface receptors have been described for the related CCN proteins, but it is now recognised that they generally act via integrin receptors with which they interact through non-classical recognition sequences [36]. Similarly, although IGFBP-3 and IGFBP-5 do not possess classical integrin recognition sequences, IGFBP-3 has been reported to associate with the β 1 integrin [35, 37], and IGFBP-3 and IGFBP-5 are know to bind with high affinity to many known integrin ligands such as fibrin, fibrinogen [38], fibronectin [39], ADAM-12 [40], plasminogen [41], thrombospondin and osteopontin [42], and to caveolin-1 and the transferrin receptor [37, 43]. It is possible that these IGFBPs interact with integrin receptors via one of these intermediates or directly via a non-classical integrin recognition sequence.…”

Section: Actions Of Igfbps Independent Of Igfsmentioning

confidence: 99%

The Role of Insulin-Like Growth Factor Binding Proteins

Holly

Perks²

2006

Neuroendocrinology

122

111

View full text Add to dashboard Cite

Insulin-like growth factors (IGFs) are fundamental cell regulators with an evolutionary conserved role synchronising tissue growth, development and function according to metabolic conditions. Although structurally very similar to insulin, the IGFs act in a very different way as cell regulators. Whereas insulin is stored in a specific gland and released when needed, the IGFs are stored outside of cells with soluble binding proteins. A very complex system of six IGF binding proteins, each of which exists in various modified states and interacts with other proteins, provides a sophisticated system for conferring specificity to provide a finely tuned system for local regulation at the tissue level.

show abstract

“…In order to determine whether the pAkt is regulated by AR mediated IGFBP3 signaling, the IGF2 inhibitor (Chromeceptin) was used to mask AR effects (Ma et al, 2011), since it has been shown that IGF2 is regulated by IGFBP3. We found pAkt is increased in ARKO BMSCs and the IGF inhibitors successfully masked AR mediated IGFBP3 signaling effects on pAkt expression in WT and ARKO BMSCs (Hashimoto et al, 1997; Oesterreicher et al, 2005; Wang et al, 2006; Xu et al, 1996) (Fig.4 H). Taken together, the results in Figure 4 clearly showed that knockout of AR suppressed IGFBP3 activation of Akt signaling and influenced the adipogenesis process.…”

Section: Resultsmentioning

confidence: 75%

Loss of androgen receptor promotes adipogenesis but suppresses osteogenesis in bone marrow stromal cells

Huang¹,

Lai²,

Luo³

et al. 2013

Stem Cell Research

View full text Add to dashboard Cite

Gender differences have been described in osteoporosis with females having a higher risk of osteoporosis than males. The differentiation of bone marrow stromal cells (BMSCs) into bone or fat is a critical step for osteoporosis. Here we demonstrated that loss of the androgen receptor (AR) in BMSCs suppressed osteogenesis but promoted adipogenesis. The mechanism dissection studies revealed that AR deficiency suppressed osteogenesis-related genes to inhibit osteoblast differentiation from BMSCs. Knockout of AR promoted adipogenesis of BMSCs via Akt activation through IGFBP3-mediated IGF signaling, and the 5′ promoter assay and chromatin immunoprecipitation assays further proved that AR could modulate IGFBP3 expression at the transcriptional level. Finally, addition of IGF inhibitors successfully masked the AR deficiency-induced Akt activation, and inhibitions of Akt, IGF1, and IGF2 pathways reversed the AR depletion effects on the adipogenesis process. These results suggested that AR-mediated changes in IGFBP3 might modulate the IGF-Akt axis to regulate adipogenesis in BMSCs.

show abstract

Interaction of Insulin-like Growth Factor II (IGF-II) with Multiple Plasma Proteins

Cited by 17 publications

References 40 publications

The IGF-II–Insulin Receptor Isoform-A Autocrine Signal in Cancer: Actionable Perspectives

The IGF-II–Insulin Receptor Isoform-A Autocrine Signal in Cancer: Actionable Perspectives

The Role of Insulin-Like Growth Factor Binding Proteins

Loss of androgen receptor promotes adipogenesis but suppresses osteogenesis in bone marrow stromal cells

Contact Info

Product

Resources

About