Recapitulation of HDV infection in a fully permissive hepatoma cell line allows efficient drug evaluation

Lempp, Florian A.; Schlund, Franziska; Rieble, Lisa; Nußbaum, Lea; Link, Corinna; Zhang, Zhenfeng; Ni, Yi; Urban, Stephan

doi:10.1038/s41467-019-10211-2

Cited by 46 publications

(75 citation statements)

References 38 publications

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“…Since HBV envelope proteins enable secretion of HBV subviral particles and support envelopment of the HDV RNPs, we stably transduced the HuH7-HDV with a lentiviral vector harboring a 2.7-kb HBV fragment encoding the HBV envelope proteins under control of their native promoter/enhancer 20 . Such a construct has also been successfully implemented in the fully replication-competent cell line HepNB2.7 16 . Following selection with blasticidin, the cell pool (referred to as HuH7-HDV-Env) secreted HBsAg as well as infectious HDV virions, as shown by quantitative HBsAg ELISA and infection of HepG2-NTCP cells using cell culture supernatants (Supplemental Fig.…”

Section: Resultsmentioning

confidence: 99%

“…pWPI-NTCP-GFP was constructed by replacing the puromycin resistance gene GFP. Plasmid pLX304-HB2.7 is a lentiviral vector expressing HBV envelope proteins 16 , which was constructed by insertion of the HBV sequence from pT7HB2.7 into the lentiviral vector pLX304 36 . The sequence of all constructs was verified by Sanger sequencing (GATC Biotech).…”

Section: Methodsmentioning

confidence: 99%

“…To study HDV secretion in vitro , current systems rely on co-transfection of hepatic cells with HDV- and HBV envelope-expressing plasmids 15 or the HepNB2.7 cell line that supports the release of progeny HDV upon infection 16 . While the HBV field has developed several virus-replicating cell lines (such as HepG2.2.15 17 and HepAD38 18 , which have been used for virus production, investigation of the viral replication cycle and identification of antiviral drug candidates), there is currently no equivalent stable cell line that supports continuous HDV replication and secretion of infectious HDV particles.…”

Section: Introductionmentioning

confidence: 99%

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Generation and characterization of a stable cell line persistently replicating and secreting the human hepatitis delta virus

Zhang

Engelskircher

et al. 2019

Sci Rep

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Human hepatitis delta virus (HDV) causes the most severe form of viral hepatitis. Approximately 15–25 million people are chronically infected with HDV. As a satellite virus of the human hepatitis B virus (HBV), HDV uses the HBV-encoded envelope proteins for egress from and de novo entry into hepatocytes. So far, in vitro production of HDV particles is restricted to co-transfection of cells with HDV/HBV encoding cDNAs. This approach has several limitations. In this study, we established HuH7-END cells, which continuously secrete infectious HDV virions. The cell line was generated through stepwise stable integration of the cDNA of the HDV antigenome, the genes for the HBV envelope proteins and the HBV/HDV receptor NTCP. We found that HuH7-END cells release infectious HDV particles up to 400 million copies/milliliter and support virus spread to co-cultured cells. Due to the expression of NTCP, HuH7-END cells are also susceptible to de novo HDV entry. Virus production is stable for >16 passages and can be scaled up for preparation of large HDV virus stocks. Finally, HuH7-END cells are suitable for screening of antiviral drugs targeting HDV replication. In summary, the HuH7-END cell line provides a novel tool to study HDV replication in vitro .

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Generation and characterization of a stable cell line persistently replicating and secreting the human hepatitis delta virus

Zhang

Engelskircher

et al. 2019

Sci Rep

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“…The three J o u r n a l P r e -p r o o f membrane-embedded HBV envelope proteins small (S-), middle (M-) and large (L-), collectively termed HBsAg, are encoded by the covalently closed circular DNA (cccDNA) in HBV replicating hepatocytes and the integrated HBV DNA in chromosomes. [21][22][23][24][25] The HDV replication cycle is depicted in Fig. 1.…”

Section: Hdv Replication Cyclementioning

confidence: 99%

“…Application of newly developed cell culture models, e.g. cell lines expressing both, the HDV receptor and the HBV envelope thereby supporting the full HDV life cycle, 23,24 will be helpful to better understand to what extend these HDV-specific countermeasures contribute to the surveillance of immune recognition. 103 Of note, the sensitivity of HDV RNA quantification assay at that time was low 104 and therefore rates of serum RNA negativation were probably overestimated.…”

Section: Viral Countermeasures To Hdv Induced Ifn Responsesmentioning

confidence: 99%

New insights into HDV persistence: The role of interferon response and implications for upcoming novel therapies

Zhang

Urban

2021

Journal of Hepatology

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A phase 2 dose‐finding study of lonafarnib and ritonavir with or without interferon alpha for chronic delta hepatitis

et al. 2021

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Background and Aims Proof‐of‐concept studies demonstrated lonafarnib (LNF), a first‐in‐class oral prenylation inhibitor, efficacy in patients infected with HDV. The lonafarnib with ritonavir for HDV‐2 (LOWR‐2) study’s aim was to identify optimal combination regimens of LNF + ritonavir (RTV) ± pegylated interferon alpha (PEG‐IFNα) with efficacy and tolerability for longer‐term dosing. Here we report the safety and efficacy at end of treatment for up to 24 weeks. Approach and Results Fifty‐five patients with chronic HDV were consecutively enrolled in an open‐label, single‐center, phase 2 dose‐finding study. There were three main treatment groups: high‐dose LNF (LNF ≥ 75 mg by mouth [po] twice daily [bid] + RTV) (n = 19, 12 weeks); all‐oral low‐dose LNF (LNF 25 or 50 mg po bid + RTV) (n = 24, 24 weeks), and combination low‐dose LNF with PEG‐IFNα (LNF 25 or 50 mg po bid + RTV + PEG‐IFNα) (n = 12, 24 weeks). The primary endpoint, ≥2 log10 decline or < lower limit of quantification of HDV‐RNA from baseline at end of treatment, was reached in 46% (6 of 13) and 89% (8 of 9) of patients receiving the all‐oral regimen of LNF 50 mg bid + RTV, and combination regimens of LNF (25 or 50 mg bid) + RTV + PEG‐IFNα, respectively. In addition, multiple patients experienced well‐tolerated transient posttreatment alanine aminotransferase increases, resulting in HDV‐RNA negativity and alanine aminotransferase normalization. The proportions of grade 2 and 3 gastrointestinal adverse events in the high‐dose versus low‐dose groups were 49% (37 of 76) and only 22% (18 of 81), respectively. Conclusions LNF, boosted with low‐dose RTV, is a promising all‐oral therapy, and maximal efficacy is achieved with PEG‐IFNα addition. The identified optimal regimens support a phase 3 study of LNF for the treatment of HDV.

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Recapitulation of HDV infection in a fully permissive hepatoma cell line allows efficient drug evaluation

Cited by 46 publications

References 38 publications

Generation and characterization of a stable cell line persistently replicating and secreting the human hepatitis delta virus

Generation and characterization of a stable cell line persistently replicating and secreting the human hepatitis delta virus

New insights into HDV persistence: The role of interferon response and implications for upcoming novel therapies

A phase 2 dose‐finding study of lonafarnib and ritonavir with or without interferon alpha for chronic delta hepatitis

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