We provide evidence that type II alveolar epithelial cells (AECIIs) respond to pulmonary infection of vaccinia virus by inducing IFN-β and IFN-stimulated genes via the activation of the MDA5 and STING-mediated nucleic acid-sensing pathways and the type I IFN positive feedback loop. Here we report that vaccinia C7 is a crucial virulence factor that blocks activation of the transcription factor IRF3. Intranasal infection of mice with vaccinia virus causes lethal pneumonia and systemic dissemination. How these immune components function during an acute poxvirus infection is not well understood. The pulmonary immune system consists of a network of tissue-resident cells as well as immune cells that are recruited to the lungs during infection and/or inflammation.
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