2012
DOI: 10.1530/erc-12-0329
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IGF1 dependence of dietary energy balance effects on murine Met1 mammary tumor progression, epithelial-to-mesenchymal transition, and chemokine expression

Abstract: Luminal breast tumors with little or no estrogen receptor a expression confer poor prognosis. Using the Met1 murine model of luminal breast cancer, we characterized the IGF1-dependency of diet-induced obesity (DIO) and calorie restriction (CR) effects on tumor growth, growth factor signaling, epithelial-to-mesenchymal transition (EMT), and chemokine expression. Liver-specific IGF1-deficient (LID) and littermate control (LC) mice were administered control, DIO, or 30% CR diets for 3 months before orthotopic inj… Show more

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Cited by 27 publications
(25 citation statements)
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“…The LID mice were then injected with NB508 PDAC cells derived from a spontaneous tumor of a Kras Ink4a +/- mouse. Previously, we used this model to establish that the effects of CR and obesity on tumor suppression or progression, respectively, were largely dependent upon modulation of circulating IGF-1 (15). In the LID mice, CR did not reduce mammary tumor growth or circulating levels of IGF-1 relative to the control diet.…”
Section: Discussionmentioning
confidence: 99%
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“…The LID mice were then injected with NB508 PDAC cells derived from a spontaneous tumor of a Kras Ink4a +/- mouse. Previously, we used this model to establish that the effects of CR and obesity on tumor suppression or progression, respectively, were largely dependent upon modulation of circulating IGF-1 (15). In the LID mice, CR did not reduce mammary tumor growth or circulating levels of IGF-1 relative to the control diet.…”
Section: Discussionmentioning
confidence: 99%
“…In the LID mice, CR did not reduce mammary tumor growth or circulating levels of IGF-1 relative to the control diet. Although DIO LID mice displayed some IGF-independent effects, these were not able to overcome the prevailing impact of low circulating IGF-1 on tumor growth (15). Consistent with a causal relationship between IGF-1 and PDAC, LID mice, relative to WT mice, had significantly reduced serum IGF-1 levels, PDAC growth, tumoral proliferation (as assessed by Ki-67 staining), and tumoral Akt/mTOR signaling; each of which was rescued by IGF-1 infusion.…”
Section: Discussionmentioning
confidence: 99%
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“…Levels of protein expression were analyzed using the Lincoplex bead-based cytokine/chemokine panel (Millipore Corporation, Billerica, MS) on a BioRad Bioplex 200 analyzer (BioRad) according to manufacturer's directions. Choice of concentration (400 ng/mL) was based on physiologically relevant levels of circulating IGF-1 observed in mice fed the same control diet used in the present study [35], [36], [37]. Supernatants were collected from three separate experiments.…”
Section: Methodsmentioning
confidence: 99%
“…Elevated IGF-1 has been identified as a risk factor in many cancer types (18). In a genetically engineered mouse model of liver-specific IGF-1 deficiency, circulating IGF-1 was reduced by ;75%, causing a significant decrease (relative to a wild-type control) in either tumor multiplicity or volume in mouse models of colon (26), mammary (27), or pancreatic (28) cancer. Liver-specific IGF-1 deficiency mice, relative to wild-type mice, also show reduced serum cytokine concentrations, and this has been linked to an IGF-1/NF-kB interaction (26).…”
Section: Obesity-related Hormones and Growth Factors And Inflammationmentioning
confidence: 99%