Complement Suppresses the Initial Type 1 Interferon Response to Ocular Herpes Simplex Virus Type 1 Infection in Mice
Daniel J. J. Carr, Adrian Filiberti, Grzegorz B. Gmyrek

TL;DR
The complement system suppresses the early immune response to a herpes virus in mice, leading to higher virus replication in the eye.
Contribution
This study reveals a novel role of the complement system in suppressing the type I interferon response during early HSV-1 infection in mice.
Findings
C3KO mice had less infectious virus in the cornea at 24 hours post-infection compared to wild-type mice.
C3KO mice showed increased type I interferon gene expression at early time points after infection.
Only CCL3 (MIP-1α) levels were significantly different between WT and C3KO mice at 12 hours post-infection.
Abstract
The complement system (CS) contributes to the initial containment of viral and bacterial pathogens and clearance of dying cells in circulation. We previously reported mice deficient in complement component 3 (C3KO mice) were more sensitive than wild-type (WT) mice to ocular HSV-1 infection, as measured by a reduction in cumulative survival and elevated viral titers in the nervous system but not the cornea between days three and seven post infection (pi). The present study was undertaken to determine if complement deficiency impacted virus replication and associated changes in inflammation at earlier time points in the cornea. C3KO mice were found to possess significantly (p < 0.05) less infectious virus in the cornea at 24 h pi that corresponded with a decrease in HSV-1 lytic gene expression at 12 and 24 h pi compared to WT animals. Flow cytometry acquisition found no differences in the…
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Taxonomy
TopicsComplement system in diseases · Herpesvirus Infections and Treatments · interferon and immune responses
