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Regulatory crosstalk and interference between the xenobiotic and hypoxia sensing pathways at the AhR-ARNT-HIF1α signaling node

机译:AhR-ARNT-HIF1α信号传导节点的异源和缺氧传感途径之间的调控串扰和干扰

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摘要

The aryl hydrocarbon receptor (AhR) is a ligand-activated transcription factor that mediates many of the responses to toxic environmental chemicals such as TCDD or dioxin-like PCBs. To regulate gene expression, the AhR requires its binding partner, the aryl hydrocarbon receptor nuclear translocator (ARNT). ARNT is also required by the hypoxia-inducible factor-1α (HIF-1α), a crucial regulator of responses to conditions of reduced oxygen. The important role of ARNT in both the AhR and HIF-1α signaling pathways establishes a meaningful foundation for a possible crosstalk between these two vitally important signaling pathways. This crosstalk might lead to interference between the two signaling pathways and thus might play a role in the variety of cellular responses after exposure to AhR ligands and reduced oxygen availability. This review focuses on studies that have analyzed the effect of low oxygen environments and hypoxiamimetic agents on AhR signaling and conversely, the effect of AhR ligands, with a special emphasis on PCBs, on HIF-1α signaling. We highlight studies that assess the role of ARNT, elucidate the mechanism of the crosstalk, and discuss the physiological implications for exposure to AhR-inducing compounds in the context of hypoxia.
机译:芳烃受体(AhR)是一种配体激活的转录因子,可介导对有毒环境化学物质(例如TCDD或二恶英样PCB)的许多响应。为了调节基因表达,AhR需要其结合伴侣,即芳烃受体核转运子(ARNT)。低氧诱导因子-1α(HIF-1α)也需要ARNT,HIF-1α是对氧气还原条件作出反应的关键调节剂。 ARNT在AhR和HIF-1α信号通路中的重要作用为这两个至关重要的信号通路之间可能的串扰建立了有意义的基础。这种串扰可能会导致这两个信号通路之间的干扰,因此可能在暴露于AhR配体和氧气利用率降低后的多种细胞反应中发挥作用。这篇综述的重点是已经分析了低氧环境和亚氨肟化剂对AhR信号的影响的研究,相反,AhR配体对HIF-1α信号的影响特别是对PCB的影响进行了分析。我们重点介绍了评估ARNT的作用,阐明串扰机制的研究,并讨论了在缺氧情况下暴露于AhR诱导化合物的生理影响。

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