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Kidney tubular transcription co-activator, Yes-associated protein 1 (YAP), controls the expression of collecting duct aquaporins and water homeostasis

Yu Zhang, Huihui Huang, Yonglun Kong, Chunhua Xu, Liujiang Dai, Xiaoqiang Geng, Yujie Deng, Yang Wang, Yang Liu, Chenling Meng, Xiaoyi Zhang, Jinhong Li, Jinzhong Qin, Bo Feng, Kingston Kinglun Mak, Li Wang, Yu Huang, Weidong Wang, Hui-Yao Lan, Baoxue YangHua A. Jenny Lu, Yin Xia*

*Corresponding author for this work

Research output: Journal Publications and ReviewsRGC 21 - Publication in refereed journalpeer-review

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Abstract

Final urine volume and concentration are defined by water reabsorption through the water channel proteins aquaporin (AQP)-2, -3 and -4 in the collecting duct. However, the transcriptional regulation of these AQPs is not well understood. The Hippo/Yes-associated protein 1 (YAP) pathway plays an important role in organ size control and tissue homeostasis. When the Hippo pathway including the Mst1/Mst2 kinases is inhibited, YAP is activated and functions as a transcription co-activator. Our previous work revealed a pathological role of tubular YAP activation in chronic kidney disease, but the physiological role of YAP in the kidney remains to be established. Here, we found that tubule-specific Yap knockout mice showed increased urine output and decreased urinary osmolality. Decreases in Aqp2, -3 and -4 mRNA and protein abundance in the kidney were evident in Yap knockout mice. Analysis of Mst1/Mst2 double knockout and Mst1/Mst2/Yap triple knockout mice showed that expression of Aqp2 and Aqp4 but not Aqp3 was dependent on YAP. Furthermore, YAP was recruited to the promoters of the Aqp2 and Aqp4 genes and stimulated their transcription. Interestingly, YAP was found to interact with transcription factors GATA2, GATA3 and NFATc1. These three factors promoted Aqp2 transcription in a YAP dependent manner in collecting duct cells. These three factors also promoted Aqp4 transcription whereas only GATA2 and GATA3 enhanced Aqp3 transcription. Thus, our results suggest that YAP promotes Aqp2 and Aqp4 transcription, interacts with GATA2, GATA3 and NFATc1 to control Aqp2 expression, while Aqp-2, -3 and -4 exploit overlapping mechanisms for their baseline transcriptional regulation. © 2022, International Society of Nephrology. Published byElsevier Inc.
Original languageEnglish
Pages (from-to)501-513
Number of pages13
JournalKidney International
Volume103
Issue number3
Online published1 Nov 2022
DOIs
Publication statusPublished - Mar 2023

Funding

The authors thank Dr. Youfei Guan (Dalian Medical University), Dr. Yingzi Yang (Harvard School of Dental Medicine), Dr. Ming-Jiun Yu (National Taiwan University), and Dr. Yuan-Xiang Tao (The State University of New Jersey) for the Aqp2-Luc, Flag-hNFATc1, V5-Elf3, and C/EBP-b plasmids, respectively. The authors are grateful to Dr. Chao Wan (The Chinese University of Hong Kong) for providing the GFP and Cre adenoviruses. The authors thank Dr. Xiangjian Zheng and Dr. Yupeng Chen (Tianjin Medical University) for helpful discussions. YZ was supported in part by a Hong Kong PhD Fellowship (HKPFS) and by The Chinese University of Hong Kong School of Biomedical Sciences Postdoctoral Fellowship. This work was supported by General Research Fund 14102620, the Hong Kong Research Grants Council (to YX), Hong Kong Research Grants Council grant SRFS2021-4S04 (to YH), and the Guangdong-Hong KongMacao-Joint Laboratory Program (2019B121205005) from Guangdong Science and Technology Department (to H-YL).

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

  1. SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well-being

Research Keywords

  • AQP2
  • AQP4
  • GATA2
  • GATA3
  • NFATc1
  • YAP

Publisher's Copyright Statement

  • This full text is made available under CC-BY-NC-ND 4.0. https://creativecommons.org/licenses/by-nc-nd/4.0/

RGC Funding Information

  • RGC-funded

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