University of Missouri-Kansas City, Kansas City, MO 64108, USA.
Br J Pharmacol. 2011 Sep;164(1):68-82. doi: 10.1111/j.1476-5381.2011.01383.x.
Peroxisome proliferator-activated receptors (PPARs), members of the nuclear hormone receptor superfamily, function as transcription factors and modulators of gene expression. These actions allow PPARs to regulate a variety of biological processes and to play a significant role in several diseases and conditions. The current literature describes frequently opposing and paradoxical roles for the three PPAR isotypes, PPARα, PPARβ/δ and PPARγ, in cancer. While some studies have implicated PPARs in the promotion and development of cancer, others, in contrast, have presented evidence for a protective role for these receptors against cancer. In some tissues, the expression level of these receptors and/or their activation correlates with a positive outcome against cancer, while, in other tissue types, their expression and activation have the opposite effect. These disparate findings raise the possibility of (i) PPAR receptor-independent effects, including effects on receptors other than PPARs by the utilized ligands; (ii) cancer stage-specific effect; and/or (iii) differences in essential ligand-related pharmacokinetic considerations. In this review, we highlight the latest available studies on the role of the various PPAR isotypes in cancer in several major organs and present challenges as well as promising opportunities in the field.
过氧化物酶体增殖物激活受体(PPARs)是核激素受体超家族的成员,作为转录因子和基因表达的调节剂发挥作用。这些作用使 PPARs 能够调节多种生物过程,并在多种疾病和病症中发挥重要作用。目前的文献描述了三种 PPAR 亚型(PPARα、PPARβ/δ 和 PPARγ)在癌症中经常存在的相反和矛盾的作用。虽然一些研究表明 PPARs 参与了癌症的促进和发展,但其他研究则为这些受体对癌症的保护作用提供了证据。在一些组织中,这些受体的表达水平及其激活与对癌症的积极结果相关,而在其他组织类型中,它们的表达和激活则具有相反的效果。这些相互矛盾的发现提出了以下可能性:(i)PPAR 受体非依赖性效应,包括所使用的配体对除 PPAR 以外的受体的效应;(ii)癌症阶段特异性效应;和/或(iii)与基本配体相关的药代动力学考虑因素的差异。在这篇综述中,我们重点介绍了关于各种 PPAR 亚型在几个主要器官中癌症作用的最新研究,并提出了该领域的挑战和有希望的机会。
