Genetic and pharmacological inhibition of XBP1 protects against APAP hepatotoxicity through the activation of autophagy

Hui Ye; Chaobo Chen; Hanghang Wu; Kang Zheng; Beatriz Martín-Adrados; Esther Caparros; Rubén Francés; Leonard J. Nelson; Manuel Gómez del Moral; Iris Asensio; Javier Vaquero; Rafael Bañares; Matías A. Ávila; Raúl J. Andrade; M. Isabel Lucena; Maria Luz Martínez-Chantar; Helen L. Reeves; Steven Masson; Richard S. Blumberg; Jordi Gracia-Sancho; Yulia A. Nevzorova; Eduardo Martínez-Naves; Francisco Javier Cubero

doi:10.1038/s41419-022-04580-8

Cell Death and Disease (Feb 2022)

Genetic and pharmacological inhibition of XBP1 protects against APAP hepatotoxicity through the activation of autophagy

Hui Ye,
Chaobo Chen,
Hanghang Wu,
Kang Zheng,
Beatriz Martín-Adrados,
Esther Caparros,
Rubén Francés,
Leonard J. Nelson,
Manuel Gómez del Moral,
Iris Asensio,
Javier Vaquero,
Rafael Bañares,
Matías A. Ávila,
Raúl J. Andrade,
M. Isabel Lucena,
Maria Luz Martínez-Chantar,
Helen L. Reeves,
Steven Masson,
Richard S. Blumberg,
Jordi Gracia-Sancho,
Yulia A. Nevzorova,
Eduardo Martínez-Naves,
Francisco Javier Cubero

Affiliations

Hui Ye: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Chaobo Chen: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Hanghang Wu: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Kang Zheng: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Beatriz Martín-Adrados: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Esther Caparros: Departmento de Medicina Clínica, Universidad Miguel Hernández
Rubén Francés: Departmento de Medicina Clínica, Universidad Miguel Hernández
Leonard J. Nelson: Institute for Bioengineering (IBioE), Human Tissue Engineering, Faraday Building, The University of Edinburgh
Manuel Gómez del Moral: Department of Cell Biology, Complutense University School of Medicine
Iris Asensio: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Javier Vaquero: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Rafael Bañares: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Matías A. Ávila: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Raúl J. Andrade: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
M. Isabel Lucena: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Maria Luz Martínez-Chantar: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Helen L. Reeves: The Liver Unit, Newcastle-upon-Tyne Hospitals NHS Foundation Trust
Steven Masson: The Liver Unit, Newcastle-upon-Tyne Hospitals NHS Foundation Trust
Richard S. Blumberg: Division of Gastroenterology, Hepatology, and Endoscopy, Department of Medicine, Brigham and Women´s Hospital, Harvard Medical School, Boston, and Harvard Digestive Diseases Center
Jordi Gracia-Sancho: Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD)
Yulia A. Nevzorova: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Eduardo Martínez-Naves: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine
Francisco Javier Cubero: Department of Immunology, Ophthalmology and ENT, Complutense University School of Medicine

DOI: https://doi.org/10.1038/s41419-022-04580-8
Journal volume & issue: Vol. 13, no. 2
pp. 1 – 13

Abstract

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Abstract Acetaminophen (APAP) hepatotoxicity induces endoplasmic reticulum (ER) stress which triggers the unfolded protein response (UPR) in hepatocytes. However, the mechanisms underlying ER stress remain poorly understood, thus reducing the options for exploring new pharmacological therapies for patients with hyperacute liver injury. Eight-to-twelve-week-old C57BL/6J Xbp1-floxed (Xbp1 f/f ) and hepatocyte-specific knockout Xbp1 mice (Xbp1 ∆hepa ) were challenged with either high dose APAP [500 mg/kg] and sacrificed at early (1–2 h) and late (24 h) stages of hepatotoxicity. Histopathological examination of livers, immunofluorescence and immunohistochemistry, Western blot, real time (RT)-qPCR studies and transmission electron microscopy (TEM) were performed. Pharmacological inhibition of XBP1 using pre-treatment with STF-083010 [STF, 75 mg/kg] and autophagy induction with Rapamycin [RAPA, 8 mg/kg] or blockade with Chloroquine [CQ, 60 mg/kg] was also undertaken in vivo. Cytoplasmic expression of XBP1 coincided with severity of human and murine hyperacute liver injury. Transcriptional and translational activation of the UPR and sustained activation of JNK1/2 were major events in APAP hepatotoxicity, both in a human hepatocytic cell line and in a preclinical model. Xbp1 ∆hepa livers showed decreased UPR and JNK1/2 activation but enhanced autophagy in response to high dose APAP. Additionally, blockade of XBP1 splicing by STF, mitigated APAP-induced liver injury and without non-specific off-target effects (e.g., CYP2E1 activity). Furthermore, enhanced autophagy might be responsible for modulating CYP2E1 activity in Xbp1 ∆hepa animals. Genetic and pharmacological inhibition of Xbp1 specifically in hepatocytes ameliorated APAP-induced liver injury by enhancing autophagy and decreasing CYP2E1 expression. These findings provide the basis for the therapeutic restoration of ER stress and/or induction of autophagy in patients with hyperacute liver injury.

Published in Cell Death and Disease

ISSN: 2041-4889 (Online)
Publisher: Nature Publishing Group
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Cytology
Website: http://www.nature.com/cddis/index.html

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