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2
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Biochim Biophys Acta Mol Basis Dis. 2021 Jan 1;1867(1):165994. doi: 10.1016/j.bbadis.2020.165994. Epub 2020 Oct 22.
3
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ZO-2 有利于 Hippo 信号通路,AMPK 在脂肪变性肝脏中的再表达可恢复连接的封闭。

ZO-2 favors Hippo signaling, and its re-expression in the steatotic liver by AMPK restores junctional sealing.

机构信息

Department of Physiology, Biophysics, and Neurosciences, Center for Research and Advanced Studies (Cinvestav), Mexico City, Mexico.

Laboratory of Molecular Cardiology, Institute of Physiology, Benemérita Universidad Autónoma de Puebla, Puebla, Mexico.

出版信息

Tissue Barriers. 2022 Apr 3;10(2):1994351. doi: 10.1080/21688370.2021.1994351. Epub 2021 Oct 23.

DOI:10.1080/21688370.2021.1994351
PMID:34689705
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9067463/
Abstract

ZO-2 is a peripheral ight unction (TJ) protein whose silencing in renal epithelia induces cell hypertrophy. Here, we found that in ZO-2 KD MDCK cells, in compensatory renal hypertrophy triggered in rats by a unilateral nephrectomy and in liver steatosis of bese ucker (OZ) rats, ZO-2 silencing is accompanied by the diminished activity of LATS, a kinase of the Hippo pathway, and the nuclear concentration of YAP, the final effector of this signaling route. ZO-2 appears to function as a scaffold for the Hippo pathway as it associates to LATS1. ZO-2 silencing in hypertrophic tissue is due to a diminished abundance of ZO-2 mRNA, and the Sp1 transcription factor is critical for ZO-2 transcription in renal cells. Treatment of OZ rats with metformin, an activator of AMPK that blocks JNK activity, augments ZO-2 and claudin-1 expression in the liver, reduces the paracellular permeability of hepatocytes, and serum bile acid content. Our results suggest that ZO-2 silencing is a common feature of hypertrophy, and that ZO-2 is a positive regulator of the Hippo pathway that regulates cell size. Moreover, our observations highlight the importance of AMPK, JNK, and ZO-2 as therapeutic targets for blood-bile barrier dysfunction.

摘要

ZO-2 是一种外周亮功能(TJ)蛋白,其在肾上皮细胞中的沉默会诱导细胞肥大。在这里,我们发现,在单侧肾切除术诱导的大鼠代偿性肾肥大和肥胖型 Zucker(OZ)大鼠的肝脂肪变性中,ZO-2 沉默伴随着 Hippo 通路激酶 LATS 的活性降低,以及该信号通路的最终效应物 YAP 的核浓度升高。ZO-2 似乎作为 Hippo 通路的支架,因为它与 LATS1 相关联。在肥大组织中,ZO-2 沉默是由于 ZO-2 mRNA 的丰度降低,而 Sp1 转录因子对于肾细胞中 ZO-2 的转录至关重要。用二甲双胍(一种激活 AMPK 并阻断 JNK 活性的药物)治疗 OZ 大鼠,可增加肝脏中 ZO-2 和 Claudin-1 的表达,降低肝细胞的旁细胞通透性和血清胆汁酸含量。我们的结果表明,ZO-2 沉默是肥大的一个共同特征,ZO-2 是调节细胞大小的 Hippo 通路的正调节剂。此外,我们的观察结果强调了 AMPK、JNK 和 ZO-2 作为治疗血液胆汁屏障功能障碍的治疗靶点的重要性。