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Research Article| Volume 71, ISSUE 4, P719-730, October 2019

Activation of YAP attenuates hepatic damage and fibrosis in liver ischemia-reperfusion injury

  • Author Footnotes
    † These authors contributed equally to this work.
    Yuan Liu
    Footnotes
    † These authors contributed equally to this work.
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA

    Department of Liver Surgery, Ren Ji Hospital Affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China
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  • Author Footnotes
    † These authors contributed equally to this work.
    Tianfei Lu
    Footnotes
    † These authors contributed equally to this work.
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA

    Department of Liver Surgery, Ren Ji Hospital Affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China
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  • Author Footnotes
    † These authors contributed equally to this work.
    Cheng Zhang
    Footnotes
    † These authors contributed equally to this work.
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA

    Department of Surgery, Division of Hepatobiliary and Pancreatic Surgery, The First Affiliated Hospital, Zhejiang University, School of Medicine, Hangzhou, Zhejiang, China
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  • Jin Xu
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA

    Department of Pancreatic Surgery, Shengjing Hospital, China Medical University, Shenyang, China
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  • Zhengze Xue
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA

    Department of Surgery, Division of Hepatobiliary and Pancreatic Surgery, The First Affiliated Hospital, Zhejiang University, School of Medicine, Hangzhou, Zhejiang, China
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  • Ronald W. Busuttil
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA
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  • Ning Xu
    Correspondence
    Corresponding authors. Addresses: Dumont-UCLA Transplant Center, 77-120 CHS, 10833 Le Conte Ave, Los Angeles, CA 90095, USA. Tel.: +1 (323) 205-5156, (H. Ji), or Department of Liver Surgery, Ren Ji Hospital affiliated to Shanghai Jiao Tong University School of Medicine, No. 160, Pujian Road, Shanghai 200127, China (Q. Xia or N. Xu).
    Affiliations
    Department of Liver Surgery, Ren Ji Hospital Affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China
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  • Qiang Xia
    Correspondence
    Corresponding authors. Addresses: Dumont-UCLA Transplant Center, 77-120 CHS, 10833 Le Conte Ave, Los Angeles, CA 90095, USA. Tel.: +1 (323) 205-5156, (H. Ji), or Department of Liver Surgery, Ren Ji Hospital affiliated to Shanghai Jiao Tong University School of Medicine, No. 160, Pujian Road, Shanghai 200127, China (Q. Xia or N. Xu).
    Affiliations
    Department of Liver Surgery, Ren Ji Hospital Affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China
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  • Jerzy W. Kupiec-Weglinski
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA
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  • Haofeng Ji
    Correspondence
    Corresponding authors. Addresses: Dumont-UCLA Transplant Center, 77-120 CHS, 10833 Le Conte Ave, Los Angeles, CA 90095, USA. Tel.: +1 (323) 205-5156, (H. Ji), or Department of Liver Surgery, Ren Ji Hospital affiliated to Shanghai Jiao Tong University School of Medicine, No. 160, Pujian Road, Shanghai 200127, China (Q. Xia or N. Xu).
    Affiliations
    Dumont-UCLA Transplant Center, Division of Liver and Pancreas Transplantation, Department of Surgery, David Geffen School of Medicine at University of California-Los Angeles, Los Angeles, CA, USA
    Search for articles by this author
  • Author Footnotes
    † These authors contributed equally to this work.
Published:June 12, 2019DOI:https://doi.org/10.1016/j.jhep.2019.05.029
Activation of YAP attenuates hepatic damage and fibrosis in liver ischemia-reperfusion injury
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      Highlights

      • High graft YAP expression was correlated with well-preserved histology and improved hepatocellular function in human OLT.
      • YAP activation promoted downstream regenerative/anti-oxidative gene induction.
      • YAP activation diminished oxidative stress, necrosis/apoptosis, and suppressed the innate inflammatory response.
      • YAP activation suppressed extracellular matrix synthesis and hepatic stellate cell activation, and stopped fibrogenesis.
      • YAP activation failed to protect Nrf2-deficient mouse livers against IR-mediated tissue damage.

      Background & Aims

      Hepatic ischemia-reperfusion injury (IRI) is a major complication of hemorrhagic shock, liver resection and transplantation. YAP, a key downstream effector of the Hippo pathway, is essential for determining cell fate and maintaining homeostasis in the liver. We aimed to elucidate its role in IRI.

      Methods

      The role of YAP/Hippo signaling was systematically studied in biopsy specimens from 60 patients after orthotopic liver transplantation (OLT), and in a mouse model of liver warm IRI. Human biopsy specimens were collected after 2–10 h of cold storage and 3 h post-reperfusion, before being screened by western blot. In the mouse model, the role of YAP was probed by activating or inhibiting YAP prior to ischemia-reperfusion.

      Results

      In human biopsies, high post-OLT YAP expression was correlated with well-preserved histology and improved hepatocellular function at postoperative day 1–7. In mice, the ischemia insult (90 min) triggered intrinsic hepatic YAP expression, which peaked at 1–6 h of reperfusion. Activation of YAP protected the liver against IR-stress, by promoting regenerative and anti-oxidative gene induction, while diminishing oxidative stress, necrosis/apoptosis and the innate inflammatory response. Inhibition of YAP aggravated hepatic IRI and suppressed repair/anti-oxidative genes. In mouse hepatocyte cultures, activating YAP prevented hypoxia-reoxygenation induced stress. Interestingly, YAP activation suppressed extracellular matrix synthesis and diminished hepatic stellate cell (HSC) activation, whereas YAP inhibition significantly delayed hepatic repair, potentiated HSC activation, and enhanced liver fibrosis at 7 days post-IRI. Notably, YAP activation failed to protect Nrf2-deficient livers against IR-mediated damage, leading to extensive fibrosis.

      Conclusion

      Our novel findings document the crucial role of YAP in IR-mediated hepatocellular damage and liver fibrogenesis, providing evidence of a potential therapeutic target for the management of sterile liver inflammation in transplant recipients.

      Lay summary

      In the clinical arm, graft YAP expression negatively correlated with liver function and tissue damage after human liver transplantation. YAP activation attenuated hepatocellular oxidative stress and diminished the innate immune response in mouse livers following ischemia-reperfusion injury. In the mouse model, YAP inhibited hepatic stellate cell activation, and abolished injury-mediated fibrogenesis up to 7 days after the ischemic insult.

      Graphical abstract

      Figure thumbnail ga1
      Graphical Abstract

      Keywords

      Linked Article

      • Myofibroblast YAP/TAZ is dispensable for liver fibrosis in mice
        Journal of HepatologyVol. 75Issue 1
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          Severe fibrosis often leads to significant mortality as a result of liver failure and cirrhosis. Recent evidence arising in the Journal of Hepatology etc. shed light on the role of the mechanosensing Hippo/YAP/TAZ pathway during hepatic fibrosis.1–5 Those studies suggested that the YAP/TAZ pathway was activated in various mouse models of liver fibrosis and in human fibrotic liver. However, conflicting data exist for both positive and negative regulation of the YAP/TAZ pathway in liver fibrogenesis.
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      • Reply to: “Myofibroblast YAP/TAZ is dispensable for liver fibrosis in mice”
        Journal of HepatologyVol. 75Issue 1
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          We thank Dr. Xu et al. for their insightful letter1 and take advantage of this reply to clarify important aspects of our article,2 in which we employed a well-established mouse model of liver ischemia-reperfusion injury (IRI) to show that activation of YAP attenuated oxidative stress and innate immune responses in liver IRI. As activation of YAP prevented hepatocellular damage in liver IRI, it further mitigated IR-mediated liver fibrosis.
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      Article info

      Publication history

      Published online: June 12, 2019
      Accepted: May 20, 2019
      Received in revised form: May 7, 2019
      Received: January 31, 2019

      Identification

      DOI: https://doi.org/10.1016/j.jhep.2019.05.029

      Copyright

      © 2019 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.

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