Abstract
The liver possesses distinct tolerogenic properties because of continuous exposure to bacterial constituents and nonpathogenic food antigen. The central immune mediators required for the generation of effective immune responses in the liver environment have not been fully elucidated. In this report, we demonstrate that the liver can indeed support effector CD8+ T cells during adenovirus infection when the T cells are primed in secondary lymphoid tissues. In contrast, when viral antigen is delivered predominantly to the liver via intravenous (IV) adenovirus infection, intrahepatic CD8+ T cells are significantly impaired in their ability to produce inflammatory cytokines and lyse target cells. Additionally, intrahepatic CD8+ T cells generated during IV adenovirus infection express elevated levels of PD-1. Notably, lower doses of adenovirus infection do not rescue the impaired effector function of intrahepatic CD8+ T cell responses. Instead, intrahepatic antigen recognition limits the generation of potent anti-viral responses at both priming and effector stages of the CD8+ T cell response and accounts for the dysfunctional CD8+ T cell response observed during IV adenovirus infection. These results also implicate that manipulation of antigen delivery will facilitate the design of improved vaccination strategies to persistent viral infection.
Highlights
The liver is a site for continual exposure to bacterial constituents and food antigens
To examine whether intrahepatic expression of foreign antigen delivered by recombinant adenovirus (rAd) vector would result in the activation of antigen specific CD8+ T cells and the subsequent development of CD8+ effector T cells, we infected C57BL/6 mice with 56108 PFU of rAd expressing the gene encoding ovalbumin (OVA) protein (AdOVA) by IV route
We introduced the same inoculum dose of Ad-OVA by subcutaneous (SubQ) route in order to initiate CD8+ T cell response through secondary lymphoid tissue presentation within the lymph nodes draining the site of virus infection
Summary
The liver is a site for continual exposure to bacterial constituents and food antigens. To prevent the generation of harmful immune responses against bacteria or innocuous food antigens, the liver evolves a way to dampen host immunity [1]. As a result of these properties, numerous hepatotropic infections including HCV, HBV, and malaria establish chronic infections in the liver compartment [8,9,10]. CD8+ T cell responses generated during viral infection in the liver with the establishment of viral persistence display a significant defect in effector function and become functionally exhausted in later stages of infection [11,12]. Enhanced levels of T cell apoptosis have been observed during chronic liver infection [13,14]
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