Cytoplasmic PXR regulates glucose metabolism by binding mRNAs and modulating their stability

Nature structural & molecular biology Pub Date : 2025-08-12 DOI:10.1038/s41594-025-01614-5

Xiaofei Wang, Zehua Wang, Sihan Li, Dhamotharan Pattarayan, Yifei Wang, Jingchen Zhai, Yu Zhang, Haolin Wang, Meishu Xu, Junjie Zhu, Junmei Wang, Xiaochao Ma, Sridhar Mani, Wen Xie, Min Zhang, Da Yang

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Abstract

Pregnane X receptor (PXR) is a nuclear receptor considered to be a master transcription factor of xenobiotic metabolism. Here, using enhanced ultraviolet crosslinking and immunoprecipitation, we show that PXR can bind mRNAs in different cancer cell lines and normal liver tissues. PXR-bound mRNAs include genes related to metabolic reprogramming and lipid metabolism. Separately from its known nuclear transcriptional function, cytoplasmic PXR binds and stabilizes mature mRNA containing C+G-enriched sequences through its zinc-finger domain. Mechanistically, cytoplasmic PXR interacts with RNH1, an RNase inhibitor, to regulate RNA stability. In colorectal cancer cells, cytoplasmic PXR facilitates glucose uptake by stabilizing SLC2A1 mRNA. This process further promotes cell proliferation and cancer development. Our study unveils a previously unknown dimension of PXR-mediated gene regulation by characterizing PXR as an RNA-binding protein important for mRNA stability in the cytoplasm.

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胞质PXR通过结合mrna并调节其稳定性来调节葡萄糖代谢

孕烷X受体（Pregnane X receptor， PXR）是一种核受体，被认为是外源代谢的主转录因子。在这里，通过增强紫外线交联和免疫沉淀，我们发现PXR可以结合不同癌细胞系和正常肝组织中的mrna。pxr结合的mrna包括与代谢重编程和脂质代谢相关的基因。除了已知的核转录功能外，胞质PXR通过其锌指结构域结合并稳定含有C+ g富集序列的成熟mRNA。从机制上讲，细胞质PXR与RNase抑制剂RNH1相互作用，以调节RNA的稳定性。在结直肠癌细胞中，细胞质PXR通过稳定SLC2A1 mRNA促进葡萄糖摄取。这一过程进一步促进了细胞增殖和癌症的发展。我们的研究揭示了PXR介导的基因调控的一个以前未知的维度，通过将PXR表征为细胞质中mRNA稳定性重要的rna结合蛋白。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Nature structural & molecular biology

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