Author: Benedetti Gassen, Rodrigo; Fazolo, Tiago; de Freitas, Deise Nascimento; Borges, Thiago J; Lima, Karina; Antunes, Géssica L; Maito, Fábio; Bueno Mendes, Daniel Ag; Báfica, André; Rodrigues, Luiz Carlos; Stein, Renato; de Souza, Ana Paula Duarte; Bonorino, Cristina
Title: IL-21 treatment recovers follicular helper T cells and neutralizing antibody production in respiratory syncytial virus infection. Cord-id: cjpxl7mn Document date: 2020_10_17
ID: cjpxl7mn
Snippet: Respiratory syncytial virus (RSV) is the major cause of lower respiratory tract infections in children under 1-year-old. RSV vaccines are currently unavailable, and children suffering from multiple reinfections by the same viral strain fail to develop protective responses. Although RSV-specific antibodies can be detected upon infection, these have limited neutralizing capacity. Follicular helper T (Tfh) cells are specialized in providing signals to B cells and help the production and affinity ma
Document: Respiratory syncytial virus (RSV) is the major cause of lower respiratory tract infections in children under 1-year-old. RSV vaccines are currently unavailable, and children suffering from multiple reinfections by the same viral strain fail to develop protective responses. Although RSV-specific antibodies can be detected upon infection, these have limited neutralizing capacity. Follicular helper T (Tfh) cells are specialized in providing signals to B cells and help the production and affinity maturation of antibodies, mainly via IL-21 secretion. In this study, we asked if RSV could inhibit Tfh responses. We observed that Tfh cells fail to upregulate IL-21 production upon RSV infection. In the lungs, RSV infection downregulated the expression of IL-21/IL-21R in Tfh cells and upregulated PD-L1 expression in DCs and B cells. PD-L1 blockade during infection recovered IL-21R expression in Tfh cells and increased the secretion of IL-21 in a DC-dependent manner. IL-21 treatment decreased RSV viral load and lung inflammation, inducing the formation of tertiary lymphoid organs (TLOs) in the lung. It also decreased regulatory follicular T cells (Tfr), and increased Tfh cells, B cells, antibody avidity, and neutralization capacity, leading to an overall improved anti-RSV humoral response in infected mice. Passive immunization with purified IgG from IL-21 treated RSV-infected mice protected against RSV infection. Our results unveil a pathway by which RSV affects Tfh cells by increasing PD-L1 expression on antigen-presenting cells (APCs), highlighting the importance of an IL-21/ PD-L1 axis for the generation of protective responses to RSV infection.
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