Review

. 2012 Jan 1;17(5):1816-34.

doi: 10.2741/4021.

PPAR gamma, bioactive lipids, and cancer progression

Gregory T Robbins¹, Daotai Nie

Affiliations

PMID: 22201838
PMCID: PMC3409468
DOI: 10.2741/4021

Review

PPAR gamma, bioactive lipids, and cancer progression

Gregory T Robbins et al. Front Biosci (Landmark Ed). 2012.

. 2012 Jan 1;17(5):1816-34.

doi: 10.2741/4021.

Authors

Gregory T Robbins¹, Daotai Nie

Affiliation

¹ Department of Medical Microbiology, Immunology and Cell Biology, Southern Illinois University School of Medicine.

PMID: 22201838
PMCID: PMC3409468
DOI: 10.2741/4021

Abstract

In this article we review the evolution of cancer research involving PPARgamma, including mechanisms, target genes, and clinical applications. For the last thirteen years, the effects of PPARgamma activity on tumor biology have been studied intensely. Most of this research has focused upon the potential for employing agonists of this nuclear receptor in cancer treatment. As a monotherapy such agonists have shown little success in clinical trials, while they have shown promise as components of combination treatments both in culture and in animal models. Other investigations have explored a possible role for PPARgamma as a tumor suppressor, and as an inducer of differentiation of cancer stem cells. Whereas early studies have yielded variable conclusions regarding the prevalence of PPARgamma mutations in cancer, the protein level of this receptor has been more recently identified as a significant prognostic marker. We predict that indicators of PPARgamma activity may also serve as predictive markers for tailoring treatments.

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Figures

**Figure 1. Bioactive lipids and PPARgamma ligands**
Naturally occurring PPARgamma ligands arising from the metabolism of arachidonic acid and linoleic acid are shown. Several of the enzymes in these pathways are associated with tumorigenesis, and some of them have well described tumor-suppressive functions.

See this image and copyright information in PMC

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PPAR gamma, bioactive lipids, and cancer progression

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