Overexpression of fatty acid synthase is associated with palmitoylation of Wnt1 and cytoplasmic stabilization of β-catenin in prostate cancer - Laboratory Investigation

Overexpression of fatty acid synthase is associated with palmitoylation of Wnt1 and cytoplasmic stabilization of β-catenin in prostate cancer - Laboratory Investigation

Fiorentino, Michelangelo;Zadra, Giorgia;Palescandolo, Emanuele;Fedele, Giuseppe;Bailey, Dyane;Fiore, Christopher;Nguyen, Paul L;Migita, Toshiro;Zamponi, Raffaella;Di Vizio, Dolores;Priolo, Carmen;Sharma, Chandan;Xie, Wanling;Hemler, Martin E;Mucci, Lorelei;Giovannucci, Edward;Finn, Stephen;Loda, Massimo;Fiorentino, Michelangelo;Zadra, Giorgia;Palescandolo, Emanuele;Fedele, Giuseppe;Bailey, Dyane;Fiore, Christopher;Nguyen, Paul L;Migita, Toshiro;Zamponi, Raffaella;Di Vizio, Dolores;Priolo, Carmen;Sharma, Chandan;Xie, Wanling;Hemler, Martin E;Mucci, Lorelei;Giovannucci, Edward;Finn, Stephen;Loda, Massimo;
laboratory investigation 2008 Vol. 88 pp. 1340-1348
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michelangelo2008laboratoryoverexpression

Abstract

Fatty acid synthase (FASN), a key metabolic enzyme for liponeogenesis highly expressed in several human cancers, displays oncogenic properties such as resistance to apoptosis and induction of proliferation when overexpressed. To date, no mechanism has been identified to explain the oncogenicity of FASN in prostate cancer. We generated immortalized prostate epithelial cells (iPrECs) overexpressing FASN, and found that 14C-acetate incorporation into palmitate synthesized de novo by FASN was significantly elevated in immunoprecipitated Wnt-1 when compared to isogenic cells not overexpressing FASN. Overexpression of FASN caused membranous and cytoplasmic β-catenin protein accumulation and activation, whereas FASN knockdown by short-hairpin RNA resulted in a reduction in the extent of β-catenin activation. Orthotopic transplantation of iPrECs overexpressing FASN in nude mice resulted in invasive tumors that overexpressed β-catenin. A strong significant association between FASN and cytoplasmic (stabilized) β-catenin immunostaining was found in 862 cases of human prostate cancer after computerized subtraction of the membranous β-catenin signal (P

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doi:10.1038/labinvest.2008.97
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