| Literature DB >> 34689705 |
Laura González-González1, Helios Gallego-Gutiérrez1, Dolores Martin-Tapia1, José Everardo Avelino-Cruz2, Christian Hernández-Guzmán1, Sergio Israel Rangel-Guerrero3, Luis Marat Alvarez-Salas3, Erika Garay1, Bibiana Chávez-Munguía4, María Concepción Gutiérrez-Ruiz5, Dinorah Hernández-Melchor6, Esther López-Bayghen6, Lorenza González-Mariscal1.
Abstract
ZO-2 is a peripheral tight junction (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 obese Zucker (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.Entities:
Keywords: Hippo pathway; Sp1; ZO-2; hypertrophy; liver steatosis; metformin
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Year: 2021 PMID: 34689705 PMCID: PMC9067463 DOI: 10.1080/21688370.2021.1994351
Source DB: PubMed Journal: Tissue Barriers ISSN: 2168-8362