Molecular Signature Predictive of Long-Term Liver Fibrosis Progression to Inform Antifibrotic Drug Development

Tongqi Qian; Naoto Fujiwara; Bhuvaneswari Koneru; Atsushi Ono; Naoto Kubota; Arun K Jajoriya; Matthew G Tung; Emilie Crouchet; Won-Min Song; Cesia Ammi Marquez; Gayatri Panda; Ayaka Hoshida; Indu Raman; Quan-Zhen Li; Cheryl Lewis; Adam Yopp; Nicole E Rich; Amit G Singal; Shigeki Nakagawa; Nicolas Goossens; Takaaki Higashi; Anna P Koh; C Billie Bian; Hiroki Hoshida; Parissa Tabrizian; Ganesh Gunasekaran; Sander Florman; Myron E Schwarz; Spiros P Hiotis; Takashi Nakahara; Hiroshi Aikata; Eisuke Murakami; Toru Beppu; Hideo Baba; Rew Warren; Sangeeta Bhatia; Masahiro Kobayashi; Hiromitsu Kumada; Austin J Fobar; Neehar D Parikh; Jorge A Marrero; Steve Hategekimana Rwema; Venugopalan Nair; Manishkumar Patel; Seunghee Kim-Schulze; Kathleen Corey; Jacqueline G O'Leary; Goran B Klintmalm; David L Thomas; Mohammed Dibas; Gerardo Rodriguez; Bin Zhang; Scott L Friedman; Thomas F Baumert; Bryan C Fuchs; Kazuaki Chayama; Shijia Zhu; Raymond T Chung; Yujin Hoshida

doi:10.1053/j.gastro.2021.12.250

Molecular Signature Predictive of Long-Term Liver Fibrosis Progression to Inform Antifibrotic Drug Development

Gastroenterology. 2022 Apr;162(4):1210-1225. doi: 10.1053/j.gastro.2021.12.250. Epub 2021 Dec 22.

Authors

Tongqi Qian¹, Naoto Fujiwara², Bhuvaneswari Koneru¹, Atsushi Ono³, Naoto Kubota¹, Arun K Jajoriya¹, Matthew G Tung⁴, Emilie Crouchet⁵, Won-Min Song⁶, Cesia Ammi Marquez¹, Gayatri Panda¹, Ayaka Hoshida¹, Indu Raman⁷, Quan-Zhen Li⁷, Cheryl Lewis⁸, Adam Yopp⁹, Nicole E Rich¹, Amit G Singal¹, Shigeki Nakagawa¹⁰, Nicolas Goossens¹¹, Takaaki Higashi¹⁰, Anna P Koh¹, C Billie Bian¹, Hiroki Hoshida¹, Parissa Tabrizian¹², Ganesh Gunasekaran¹², Sander Florman¹², Myron E Schwarz¹², Spiros P Hiotis¹², Takashi Nakahara³, Hiroshi Aikata³, Eisuke Murakami³, Toru Beppu⁹, Hideo Baba⁹, Rew Warren¹³, Sangeeta Bhatia¹³, Masahiro Kobayashi¹⁴, Hiromitsu Kumada¹⁴, Austin J Fobar¹⁵, Neehar D Parikh¹⁵, Jorge A Marrero¹⁶, Steve Hategekimana Rwema⁴, Venugopalan Nair¹⁷, Manishkumar Patel¹⁷, Seunghee Kim-Schulze¹⁷, Kathleen Corey⁴, Jacqueline G O'Leary¹⁸, Goran B Klintmalm¹⁹, David L Thomas²⁰, Mohammed Dibas²¹, Gerardo Rodriguez²¹, Bin Zhang⁶, Scott L Friedman¹⁷, Thomas F Baumert²², Bryan C Fuchs²³, Kazuaki Chayama²⁴, Shijia Zhu²⁵, Raymond T Chung²⁶, Yujin Hoshida²⁷

Affiliations

¹ Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas.
² Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas; Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan.
³ Department of Gastroenterology and Metabolism, Graduate School of Biomedical and Health Sciences, Hiroshima University, Hiroshima, Japan.
⁴ Department of Medicine, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts.
⁵ Institut de Recherche sur les Maladies Virales et Hépatiques, Inserm U1110, University of Strasbourg, Strasbourg, France.
⁶ Department of Genetics and Genomic Sciences, Icahn School of Medicine at Mount Sinai, New York, New York.
⁷ Microarray Core Facility, Department of Immunology, BioCenter, University of Texas Southwestern Medical Center, Dallas, Texas.
⁸ Simmons Comprehensive Cancer Center, University of Texas Southwestern Medical Center, Dallas, Texas.
⁹ Department of Surgery, University of Texas Southwestern Medical Center, Dallas, Texas.
¹⁰ Department of Gastroenterological Surgery, Graduate School of Medical Sciences, Kumamoto University, Kumamoto, Japan.
¹¹ Division of Gastroenterology and Hepatology, Geneva University Hospital, Switzerland.
¹² Department of Surgery, Icahn School of Medicine at Mount Sinai, New York, New York.
¹³ Massachusetts Institute of Technology, Boston, Massachusetts.
¹⁴ Department of Hepatology, Toranomon Hospital, Tokyo, Japan.
¹⁵ Division of Gastroenterology and Hepatology, University of Michigan, Ann Arbor, Michigan.
¹⁶ Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas; Division of Gastroenterology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.
¹⁷ Department of Medicine, Icahn School of Medicine at Mount Sinai, New York, New York.
¹⁸ Dallas VA Medical Center, Dallas, Texas.
¹⁹ Baylor Simmons Transplant Institute, Dallas, Texas.
²⁰ Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland.
²¹ AbbVie, Inc, Irvine, California.
²² Institut de Recherche sur les Maladies Virales et Hépatiques, Inserm U1110, University of Strasbourg, Strasbourg, France; Institut Hospitalo-Universitaire, Pole hépato-digestif, Strasbourg University Hospitals, Strasbourg, France.
²³ Department of Surgery, Massachusetts General Hospital, Boston, Massachusetts; Ferring Pharmaceuticals, San Diego, California.
²⁴ Collaborative Research Laboratory of Medical Innovation, Research Center for Hepatology and Gastroenterology, Hiroshima University, Hiroshima, Japan; RIKEN Center for Integrative Medical Sciences, Yokohama, Japan.
²⁵ Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas. Electronic address: Shijia.Zhu@UTSouthwestern.edu.
²⁶ Department of Medicine, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts. Electronic address: chung.raymond@mgh.harvard.edu.
²⁷ Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas. Electronic address: Yujin.Hoshida@UTSouthwestern.edu.

Abstract

Background & aims: There is a major unmet need to assess the prognostic impact of antifibrotics in clinical trials because of the slow rate of liver fibrosis progression. We aimed to develop a surrogate biomarker to predict future fibrosis progression.

Methods: A fibrosis progression signature (FPS) was defined to predict fibrosis progression within 5 years in patients with hepatitis C virus and nonalcoholic fatty liver disease (NAFLD) with no to minimal fibrosis at baseline (n = 421) and was validated in an independent NAFLD cohort (n = 78). The FPS was used to assess response to 13 candidate antifibrotics in organotypic ex vivo cultures of clinical fibrotic liver tissues (n = 78) and cenicriviroc in patients with nonalcoholic steatohepatitis enrolled in a clinical trial (n = 19, NCT02217475). A serum protein-based surrogate FPS was developed and tested in a cohort of compensated cirrhosis patients (n = 122).

Results: A 20-gene FPS was defined and validated in an independent NAFLD cohort (adjusted odds ratio, 10.93; area under the receiver operating characteristic curve, 0.86). Among computationally inferred fibrosis-driving FPS genes, BCL2 was confirmed as a potential pharmacologic target using clinical liver tissues. Systematic ex vivo evaluation of 13 candidate antifibrotics identified rational combination therapies based on epigallocatechin gallate, which were validated for enhanced antifibrotic effect in ex vivo culture of clinical liver tissues. In patients with nonalcoholic steatohepatitis treated with cenicriviroc, FPS modulation was associated with 1-year fibrosis improvement accompanied by suppression of the E2F pathway. Induction of the PPARα pathway was absent in patients without fibrosis improvement, suggesting a benefit of combining PPARα agonism to improve the antifibrotic efficacy of cenicriviroc. A 7-protein serum protein-based surrogate FPS was associated with the development of decompensation in cirrhosis patients.

Conclusion: The FPS predicts long-term fibrosis progression in an etiology-agnostic manner, which can inform antifibrotic drug development.

Keywords: Companion Biomarker; Drug Development; Liver Fibrosis; Prognostic Prediction.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Disease Progression
Drug Development
Fibrosis
Humans
Liver / pathology
Liver Cirrhosis / complications
Non-alcoholic Fatty Liver Disease* / drug therapy
Non-alcoholic Fatty Liver Disease* / genetics
PPAR alpha / genetics

Molecular Signature Predictive of Long-Term Liver Fibrosis Progression to Inform Antifibrotic Drug Development

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