HIF1α-mediated RelB/APOBEC3B downregulation allows Hepatitis B Virus persistence.

[en] New therapeutic strategies against Hepatitis B virus (HBV) focus, among others, on the activation of the immune system to enable the infected host to eliminate HBV. Hypoxia inducible factor 1 alpha (HIF1α) stabilisation has been associated with impaired immune responses. HBV pathogenesis triggers chronic hepatitis-related scaring, leading inter alia to modulation of liver oxygenation and transient immune activation, both factors playing a role in HIF1α stabilisation. We addressed whether HIF1α interferes with immune-mediated induction of the cytidine deaminase APOBEC3B and subsequent covalently closed circular DNA (cccDNA) decay. Liver biopsies of chronic HBV patients (CHB) were analysed by IHC, and in situ hybridization. The effect of HIF1α induction/stabilisation on differentiated HepaRG or mice +/- HBV +/- LTβR-agonist (BS1) was assessed in vitro and in vivo. Induction of A3B and subsequent effects were analysed by RT-qPCR, immunoblotting, ChIP, ICC, and mass-spectrometry. Analysing CHB highlighted that areas with high HIF1α levels and low A3B expression correlated with high HBcAg, potentially representing a reservoir for HBV survival in immune-active patients. In vitro, HIF1α stabilisation, strongly impaired A3B expression and anti-HBV effect. Interestingly, HIF1α knock-down was sufficient to rescue the inhibition of A3B-upregulation and -mediated antiviral effects, whereas HIF2α knock-down had no effect. HIF1α stabilisation decreased the level of RelB protein but not its mRNA, which was confirmed in vivo. Noteworthy, this function of HIF1α was independent of its partner ARNT. In conclusion, inhibiting HIF1α expression or stabilisation represents a novel anti-HBV strategy in the context of immune-mediated A3B induction. High HIF1α, mediated by hypoxia or inflammation, offers a reservoir for HBV survival in vivo, and should be considered as a restricting factor in the development of novel immune therapies.

Disciplines :

Immunology & infectious disease

Author, co-author :

Riedl, Tobias

Faure-Dupuy, Suzanne

Rolland, Maude ; Université de Liège - ULiège > GIGA I3 - Molecular Immunology and Signal Transduction

Schuehle, Svenja

Hizir, Zohier

Calderazzo, Silvia

Zhuang, Xiaodong

Wettengel, Jochen

Lopez, Martin ; Université de Liège - ULiège > GIGA I3 - Molecular Immunology and Signal Transduction

Barnault, Romain

More authors (15 more)

^✱ These authors have contributed equally to this work.

Language :

English

Title :

HIF1α-mediated RelB/APOBEC3B downregulation allows Hepatitis B Virus persistence.

Publication date :

2021

Journal title :

Hepatology (Baltimore, Md.)

ISSN :

0270-9139

eISSN :

1527-3350

Peer reviewed :

Peer reviewed

European Projects :

FP7 - 321529 - INFECT-ERA - Coordination of European funding for infectious diseases research

Funders :

CE - Commission Européenne [BE]
Union Européenne [BE]

Commentary :

Available on ORBi :

since 19 May 2021

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Bibliography

https://www.who.int/news-room/fact-sheets/detail/hepatitis-b. Accessed August 2021.
Fanning GC, Zoulim F, Hou J, Bertoletti A. Therapeutic strategies for hepatitis B virus infection: towards a cure. Nat Rev Drug Discov 2019;18:827-844.
Lucifora J, Bonnin M, Aillot L, Fusil F, Maadadi S, Dimier L, et al. Direct antiviral properties of TLR ligands against HBV replication in immune-competent hepatocytes. Sci Rep 2018;8:5390.
Du K, Liu J, Broering R, Zhang X, Yang D, Dittmer U, et al. Recent advances in the discovery and development of TLR ligands as novel therapeutics for chronic HBV and HIV infections. Expert Opin Drug Discov 2018;13:661-670.
Niu C, Li LI, Daffis S, Lucifora J, Bonnin M, Maadadi S, et al. Toll-like receptor 7 agonist GS-9620 induces prolonged inhibition of HBV via a type I interferon-dependent mechanism. J Hepatol 2018;68:922-931.
Lucifora J, Xia Y, Reisinger F, Zhang K, Stadler D, Cheng X, et al. Specific and nonhepatotoxic degradation of nuclear hepatitis B virus cccDNA. Science 2014;343:1221-1228.
Koh S, Kah J, Tham CYL, Yang N, Ceccarello E, Chia A, et al. Nonlytic lymphocytes engineered to express virus-specific T-cell receptors limit HBV infection by activating APOBEC3. Gastroenterology 2018;155:180-193.e6.
Covino DA, Gauzzi MC, Fantuzzi L. Understanding the regulation of APOBEC3 expression: current evidence and much to learn. J Leukoc Biol 2018;103:433-444.
Wang D, Li X, Li J, Lu Y, Zhao S, Tang X, et al. APOBEC3B interaction with PRC2 modulates microenvironment to promote HCC progression. Gut 2019;68:1846-1857.
Dejardin E. The alternative NF-kappaB pathway from biochemistry to biology: pitfalls and promises for future drug development. Biochem Pharmacol 2006;72:1161-1179.
Dejardin E, Droin NM, Delhase M, Haas E, Cao Y, Makris C, et al. The lymphotoxin-β receptor induces different patterns of gene expression via two NF-κB pathways. Immunity 2002;17:525-535.
Mitchell S, Vargas J, Hoffmann A. Signaling via the NFκB system. Wiley Interdiscip Rev Syst Biol Med 2016;8:227-241.
D’Ignazio L, Bandarra D, Rocha S. NF-κB and HIF crosstalk in immune responses. FEBS J 2016;283:413-424.
Balamurugan K. HIF-1 at the crossroads of hypoxia, inflammation, and cancer. Int J Cancer 2016;138:1058-1066.
Gripon P, Rumin S, Urban S, Le Seyec J, Glaise D, Cannie I, et al. Infection of a human hepatoma cell line by hepatitis B virus. Proc Natl Acad Sci U S A 2002;99:15655-15660.
Lucifora J, Arzberger S, Durantel D, Belloni L, Strubin M, Levrero M, et al. Hepatitis B virus X protein is essential to initiate and maintain virus replication after infection. J Hepatol 2011;55:996-1003.
Seitz S, Iancu C, Volz T, Mier W, Dandri M, Urban S, et al. A slow maturation process renders hepatitis B virus infectious. Cell Host Microbe 2016;20:25-35.
Faure-Dupuy S, Delphin M, Aillot L, Dimier L, Lebossé F, Fresquet J, et al. Hepatitis B virus-induced modulation of liver macrophage function promotes hepatocyte infection. J Hepatol 2019;71:1086-1098.
Isorce N, Testoni B, Locatelli M, Fresquet J, Rivoire M, Luangsay S, et al. Antiviral activity of various interferons and pro-inflammatory cytokines in non-transformed cultured hepatocytes infected with hepatitis B virus. Antiviral Res 2016;130:36-45.
Haybaeck J, Zeller N, Wolf MJ, Weber A, Wagner U, Kurrer MO, et al. A lymphotoxin-driven pathway to hepatocellular carcinoma. Cancer Cell 2009;16:295-308.
Bersten DC, Sullivan AE, Peet DJ, Whitelaw ML. bHLH-PAS proteins in cancer. Nat Rev Cancer 2013;13:827-841.
Millet P, McCall C, Yoza B. RelB: an outlier in leukocyte biology. J Leukoc Biol 2013;94:941-951.
Wright CW, Duckett CS. The aryl hydrocarbon nuclear translocator alters CD30-mediated NF-kappaB-dependent transcription. Science 2009;323:251-255.
Gradin K, McGuire J, Wenger RH, Kvietikova I, Whitelaw ML, Toftgård R, et al. Functional interference between hypoxia and dioxin signal transduction pathways: competition for recruitment of the Arnt transcription factor. Mol Cell Biol 1996;16:5221-5231.
Palazon A, Goldrath AW, Nizet V, Johnson RS. HIF transcription factors, inflammation, and immunity. Immunity 2014;41:518-528.
Baud V, Collares D. Post-translational modifications of RelB NF-κB subunit and associated functions. Cells 2016;5:22.
Villa J, Chiu D, Brandes A, Escorcia F, Villa C, Maguire W, et al. Nontranscriptional role of Hif-1α in activation of γ-secretase and notch signaling in breast cancer. Cell Rep 2014;8:1077-1092.
Fallah J, Rini BI. HIF inhibitors: status of current clinical development. Curr Oncol Rep 2019;21:6.