Ray S, Swanson H I
Biogen Inc, Cambridge, MA 02142, USA.
Biochem Pharmacol. 2009 Feb 15;77(4):681-8. doi: 10.1016/j.bcp.2008.11.022. Epub 2008 Nov 27.
Activation of the aryl hydrocarbon receptor (AHR) by the agonist, 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) has been shown to promote tumor formation in both liver and skin. In the liver, but not the skin, the AHR-mediated events that contribute to TCDD's tumor promoting activities have been studied in some detail and are thought to involve perturbation of cell fate processes. However, studies performed using cultured cells have often resulted in apparent contradictory results indicating that the impact of TCDD on cell fate processes may be cell context dependent. We and others have shown that in primary cultured keratinocytes TCDD increases post-confluent proliferation and increases late differentiation. Further, our studies performed in these cells indicate that TCDD can also inhibit culture-induced senescence. While senescence, a permanent cell cycle arrest, is emerging as an important process regulated by oncogenes and considered to be of therapeutic importance, its role with respect to TCDD/AHR mediated tumor promotion has not been fully considered. The intent of this article is to focus primarily on senescence as a cell process relevant to skin tumorigenesis and explore the idea that the inhibition of senescence by TCDD could be an important mechanism by which it may exert its tumor promoting effects in the skin.
激动剂2,3,7,8-四氯二苯并对二恶英(TCDD)激活芳烃受体(AHR)已被证明会促进肝脏和皮肤中的肿瘤形成。在肝脏而非皮肤中,已经对AHR介导的促成TCDD肿瘤促进活性的事件进行了一些详细研究,并且认为这些事件涉及细胞命运过程的扰动。然而,使用培养细胞进行的研究常常得出明显相互矛盾的结果,这表明TCDD对细胞命运过程的影响可能取决于细胞环境。我们和其他人已经表明,在原代培养的角质形成细胞中,TCDD会增加汇合后增殖并增加晚期分化。此外,我们在这些细胞中进行的研究表明,TCDD还可以抑制培养诱导的衰老。虽然衰老,即永久性细胞周期停滞,正成为一种由癌基因调节的重要过程并被认为具有治疗重要性,但其在TCDD/AHR介导的肿瘤促进方面的作用尚未得到充分考虑。本文的目的主要是关注衰老作为与皮肤肿瘤发生相关的细胞过程,并探讨TCDD对衰老的抑制可能是其在皮肤中发挥肿瘤促进作用的重要机制这一观点。