Title (en)
Dose-Dependent Hepacivirus Infection Reveals Linkage between Infectious Dose and Immune Response
Language
English
Description (en)
More than 70 million people worldwide are still infected with the hepatitis C virus 30 years after its discovery, underscoring the need for a vaccine. To develop an effective prophylactic vaccine, detailed knowledge of the correlates of protection and an immunocompetent surrogate model are needed. In this study, we describe the minimum dose required for robust equine hepacivirus (EqHV) infection in equids and examined how this relates to duration of infection, seroconversion, and transcriptomic responses. To investigate mechanisms of hepaciviral persistence, immune response, and immune-mediated pathology, we inoculated eight EqHV naive horses with doses ranging from 1-2 copies to 1.3 × 106 RNA copies per inoculation. We characterized infection kinetics, pathology, and transcriptomic responses via next generation sequencing. The minimal infectious dose of EqHV in horses was estimated at 13 RNA copies, whereas 6 to 7 copies were insufficient to cause infection. Peak viremia did not correlate with infectious dose, while seroconversion and duration of infection appeared to be affected. Notably, seroconversion was undetectable in the low-dose infections within the surveillance period (40 to 50 days). In addition, transcriptomic analysis revealed a nearly dose-dependent effect, with greater immune activation and inflammatory response observed in high-dose infections than in low-dose infections. Interestingly, inoculation with 6-7 copies of RNA that did not result in productive infection, but was associated with a strong immune response, similar to that observed in the high-dose infections. IMPORTANCE We demonstrate that the EqHV dose of infection plays an important role for inducing immune responses, possibly linked to early clearance in high-dose and prolonged viremia in low-dose infections. In particular, pathways associated with innate and adaptive immune responses, as well as inflammatory responses, were more strongly upregulated in high-dose infections than in lower doses. Hence, inoculation with low doses may enable EqHV to evade strong immune responses in the early phase and therefore promote robust, long-lasting infection.
Keywords (en)
Hepatitis-C Virus; T-Cell Responses; Nonprimate Hepacivirus; Hcv; Chimpanzees; Clearance; Viremia; Seroconversion; Transmission; Prevalence
DOI
10.1128/spectrum.01686-22
Author of the digital object
André Gömer (Ruhr University Bochum / University of Veterinary Medicine Hannover)
Daniel Todt (Ruhr University Bochum)
Eike Steinmann (Ruhr University Bochum)
Karsten Feige (University of Veterinary Medicine Hannover)
Jessika M. V. Cavalleri (University of Veterinary Medicine Vienna)
Wolfgang Baumgärtner (University of Veterinary Medicine Hannover)
Birthe Reinecke (Twincore Centre for Experimental and Clinical Infection Research)
Maximilian K. Nocke (Ruhr University Bochum)
Christina Puff (University of Veterinary Medicine Hannover)
Julien Delarocque (University of Veterinary Medicine Hannover)
Format
application/pdf
Size
770.7 kB
Licence Selected
Type of publication
Article
Name of Publication (en)
Microbiology Spectrum
Pages or Volume
13
Volume
10
Number
5
Publisher
American Society for Microbiology
Publication Date
2022
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Persistent identifier
DOI
https://phaidra.vetmeduni.ac.at/o:2072
https://doi.org/10.1128/spectrum.01686-22 - Content
- DetailsObject typePDFDocumentFormatapplication/pdfCreated05.09.2023 01:38:33 UTC
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