Abstract
BackgroundAlthough multiple studies have demonstrated a role for exosomes during virus infections, our understanding of the mechanisms by which exosome exchange regulates immune response during viral infections and affects viral pathogenesis is still in its infancy. In particular, very little is known for cytoplasmic single-stranded RNA viruses such as SARS-CoV-2 and Rift Valley fever virus (RVFV). We have used RVFV infection as a model for cytoplasmic single-stranded RNA viruses to address this gap in knowledge. RVFV is a highly pathogenic agent that causes RVF, a zoonotic disease for which no effective therapeutic or approved human vaccine exist.ResultsWe show here that exosomes released from cells infected with RVFV (designated as EXi-RVFV) serve a protective role for the host and provide a mechanistic model for these effects. Our results show that treatment of both naïve immune cells (U937 monocytes) and naïve non-immune cells (HSAECs) with EXi-RVFV induces a strong RIG-I dependent activation of IFN-B. We also demonstrate that this strong anti-viral response leads to activation of autophagy in treated cells and correlates with resistance to subsequent viral infection. Since we have shown that viral RNA genome is associated with EXi-RVFV, RIG-I activation might be mediated by the presence of packaged viral RNA sequences.ConclusionsUsing RVFV infection as a model for cytoplasmic single-stranded RNA viruses, our results show a novel mechanism of host protection by exosomes released from infected cells (EXi) whereby the EXi activate RIG-I to induce IFN-dependent activation of autophagy in naïve recipient cells including monocytes. Because monocytes serve as reservoirs for RVFV replication, this EXi-RVFV-induced activation of autophagy in monocytes may work to slow down or halt viral dissemination in the infected organism. These findings offer novel mechanistic insights that may aid in future development of effective vaccines or therapeutics, and that may be applicable for a better molecular understanding of how exosome release regulates innate immune response to other cytoplasmic single-stranded RNA viruses.
Highlights
Rift Valley Fever (RVF) is an arthropod-borne zoonotic disease responsible for epidemics in Africa and the Arabian Peninsula
These results suggest a model in which viral RNA genome segments carried by the exosomes released from infected cells (EXi)-Rift Valley fever virus (RVFV) boost the host response to RVFV infection by RIG-I-dependent activation of the IFN pathway, enabling naïve recipient cells to fight off infection upon encountering RVFV through increased autophagic activity
We found that both the exosomes originating from uninfected cells and from RVFV-infected cells migrate mainly between the 1.08 g/ml and 1.15 g/ml density fractions, as demonstrated by the presence of the well-established exosome marker CD63 (Fig. 1A)
Summary
Rift Valley Fever (RVF) is an arthropod-borne zoonotic disease responsible for epidemics in Africa and the Arabian Peninsula. The causative agent, Rift Valley Fever virus (RVFV; Bunyavirales: Phenuiviridae), primarily utilizes a mosquito vector to infect both humans and ruminants [1]. RVF causes near 100% abortion rates in pregnant ruminants and can be fatal in humans [2]. Very little is known for cytoplasmic single-stranded RNA viruses such as SARS-CoV-2 and Rift Valley fever virus (RVFV). We have used RVFV infection as a model for cytoplasmic single-stranded RNA viruses to address this gap in knowledge. RVFV is a highly pathogenic agent that causes RVF, a zoonotic disease for which no effective therapeutic or approved human vaccine exist
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