Obesity and prostate cancer: gene expression signature of human periprostatic adipose tissue

Ricardo Ribeiro; Cátia Monteiro; Victoria Catalán; Pingzhao Hu; Virgínia Cunha; Amaia Rodrı́guez; Javier Gómez‐Ambrosi; Avelino Fraga; Paulo Príncipe; Carlos Lobato; Francisco S. N. Lobo; António Morais; Vitor Silva; José Sanches-Magalhães; Jorge Oliveira; Francisco Pina; Carlos Lopes; Rui Medeiros; Gema Frühbeck

doi:10.1186/1741-7015-10-108

Obesity and prostate cancer: gene expression signature of human periprostatic adipose tissue

Ricardo Ribeiro(Instituto Português de Oncologia Francisco Gentil), Cátia Monteiro(Portuguese League Against Epilepsy), Victoria Catalán(Instituto de Salud Carlos III), Pingzhao Hu(Hospital for Sick Children), Virgínia Cunha(Portuguese League Against Epilepsy), Amaia Rodrı́guez(Instituto de Salud Carlos III), Javier Gómez‐Ambrosi(Instituto de Salud Carlos III), Avelino Fraga(Universidade do Porto), Paulo Príncipe(CUF Porto Hospital), Carlos Lobato, Francisco S. N. Lobo(Instituto Português de Oncologia Francisco Gentil), António Morais(Instituto Português de Oncologia Francisco Gentil), Vitor Silva(Instituto Português de Oncologia Francisco Gentil), José Sanches-Magalhães(Instituto Português de Oncologia Francisco Gentil), Jorge Oliveira(Instituto Português de Oncologia Francisco Gentil), Francisco Pina(Hospital de São João), Carlos Lopes(Universidade do Porto), Rui Medeiros(Fernando Pessoa University), Gema Frühbeck(Instituto de Salud Carlos III)

BMC Medicine

September 25, 2012

10.1186/1741-7015-10-108

Cited by 93Open Access

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Abstract

BACKGROUND: Periprostatic (PP) adipose tissue surrounds the prostate, an organ with a high predisposition to become malignant. Frequently, growing prostatic tumor cells extend beyond the prostatic organ towards this fat depot. This study aimed to determine the genome-wide expression of genes in PP adipose tissue in obesity/overweight (OB/OW) and prostate cancer patients. METHODS: Differentially expressed genes in human PP adipose tissue were identified using microarrays. Analyses were conducted according to the donors' body mass index characteristics (OB/OW versus lean) and prostate disease (extra prostatic cancer versus organ confined prostate cancer versus benign prostatic hyperplasia). Selected genes with altered expression were validated by real-time PCR. Ingenuity Pathway Analysis (IPA) was used to investigate gene ontology, canonical pathways and functional networks. RESULTS: In the PP adipose tissue of OB/OW subjects, we found altered expression of genes encoding molecules involved in adipogenic/anti-lipolytic, proliferative/anti-apoptotic, and mild immunoinflammatory processes (for example, FADS1, down-regulated, and LEP and ANGPT1, both up-regulated). Conversely, in the PP adipose tissue of subjects with prostate cancer, altered genes were related to adipose tissue cellular activity (increased cell proliferation/differentiation, cell cycle activation and anti-apoptosis), whereas a downward impact on immunity and inflammation was also observed, mostly related to the complement (down-regulation of CFH). Interestingly, we found that the microRNA MIRLET7A2 was overexpressed in the PP adipose tissue of prostate cancer patients. CONCLUSIONS: Obesity and excess adiposity modified the expression of PP adipose tissue genes to ultimately foster fat mass growth. In patients with prostate cancer the expression profile of PP adipose tissue accounted for hypercellularity and reduced immunosurveillance. Both findings may be liable to promote a favorable environment for prostate cancer progression.

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