BES2005 Oral Communications Oral Communication 1: Diabetes and metabolism (9 abstracts)
Effect of cholesterol depletion on IGF-induced cell survival: the role of caveolar and non-caveolar domains
LC Matthews 1 , MJ Taggart 2 & M Westwood 1
1Department of Endocrine Sciences, University of Manchester, Manchester, UK; 2Maternal & Fetal Health Research Centre, University of Manchester, Manchester, UK.
The insulin-like growth factors (IGFs) are important regulators of cellular function, with effects on growth, survival and metabolism mediated primarily through the type 1 IGF receptor (IGFIR). Recent work suggested that localisation of IGFIR to a subset of lipid rafts, known as caveolae, may be important for IGF function. In this study we have investigated whether these membrane domains were involved in IGF-I-mediated cell survival by comparing signalling in caveolae-positive fibroblasts (NWTb3) and caveolae-negative hepatocytes (HepG2).
Subcellular fractionation (n=3) and co-immunoprecipitation (n=3) of NWTb3 cells demonstrated that the IGFIR associated with caveolin, a marker for caveolae. Assessment of nuclear morphology demonstrated that 5nM IGF-I was able to protect NWTb3 cells from apoptosis induced by 24hr serum withdrawal, with a reduction from 41.6 plus/minus 1.6% to 6.1 plus/minus 0.4% apoptosis in the presence of IGF-I (p<0.05, n=4). When caveolae were disrupted, using 5mM methyl-cyclodextrin (MCD) to sequester membrane cholesterol, IGF-I-stimulated cell survival was significantly impaired (IGF-I 6.1 plus/minus 0.4%; IGF-I, MCD 27.1 plus/minus 1.0%; n=4), even though methyl-cyclodextrin alone had no effect.
Treatment with LY294002, a PI-3K inhibitor suggested that IGF-induced cell survival was mediated through the PI-3K/PKB pathway (p<0.05, n=4). Immunoblot analysis demonstrated a reduction in IGF-I-mediated activation of PKB in cells pre-treated with methyl-cyclodextrin (n=3), which suggests that methyl-cyclodextrin may impair IGF-induced cell survival by inhibiting activation of PKB.
When experiments were conducted in cells shown to be caveolin-deficient (HepG2), methyl-cyclodextrin had the same effect on IGF-induced PKB phosphorylation (n=3) and cell survival (IGF-I 1.3 plus/minus 0.2%; IGF-I, MCD 2.6 plus/minus 0.2%, n=4) as observed in caveolin-positive NWTb3 cells. This suggests that whilst IGFIR associates with caveolin, the interaction between IGFIR and caveolin may not be obligatory for IGF signalling.
Article tools
My recent searches
My recently viewed abstracts
Endocrine Abstracts
ISSN 1470-3947 (print) | ISSN 1479-6848 (online)
© Bioscientifica 2024 |
Privacy policy |
Cookie settings
BiosciAbstracts
Bioscientifica Abstracts is the gateway to a series of products that provide a permanent, citable record of abstracts for biomedical and life science conferences.
Find out more