Student and Faculty Publications
Publication Date
8-3-2023
Journal
Nature Communications
Abstract
Chikungunya virus (CHIKV) infection has been associated with severe cardiac manifestations, yet, how CHIKV infection leads to heart disease remains unknown. Here, we leveraged both mouse models and human primary cardiac cells to define the mechanisms of CHIKV heart infection. Using an immunocompetent mouse model of CHIKV infection as well as human primary cardiac cells, we demonstrate that CHIKV directly infects and actively replicates in cardiac fibroblasts. In immunocompetent mice, CHIKV is cleared from cardiac tissue without significant damage through the induction of a local type I interferon response from both infected and non-infected cardiac cells. Using mice deficient in major innate immunity signaling components, we found that signaling through the mitochondrial antiviral-signaling protein (MAVS) is required for viral clearance from the heart. In the absence of MAVS signaling, persistent infection leads to focal myocarditis and vasculitis of the large vessels attached to the base of the heart. Large vessel vasculitis was observed for up to 60 days post infection, suggesting CHIKV can lead to vascular inflammation and potential long-lasting cardiovascular complications. This study provides a model of CHIKV cardiac infection and mechanistic insight into CHIKV-induced heart disease, underscoring the importance of monitoring cardiac function in patients with CHIKV infections.
Keywords
Animals, Humans, Mice, Chikungunya Fever, Chikungunya virus, Communicable Diseases, Disease Models, Animal, Heart Diseases, Inflammation, Persistent Infection, Vasculitis, Virus Replication, Viral pathogenesis, Alphaviruses, Mouse, RNA sequencing
Included in
Cardiology Commons, Cardiovascular Diseases Commons, Laboratory Medicine Commons, Medical Pathology Commons
Comments
PMID: 37537212