PD-1 blockade augments humoral immunity through ICOS-mediated CD4+ T cell instruction
Meiyu Zhang, Liliang Xia, Yi Yang, Shuai Liu, Ping Ji, Shujun Wang, Yingying Chen, Zhiduo Liu, Yanyun Zhang, Shun Lu, Ying Wang
Journal:INTERNATIONAL IMMUNOPHARMACOLOGY
IF:3.12
DOI:10.1016/j.intimp.2018.10.045
PMID:30448635
Published:2018-11-16
research field:分子生物学癌症研究免疫学
Abstract
Successful applications of PD-1/PD-L1 blockade in multiple cancers highlight the efficacy of immunotherapy mediated by enhancing CD8 + T cell immunity both in mouse and human. How PD-1 blockade affects humoral immunity remains unclear. Herein we demonstrated that treatment of anti-PD-1 antibody led to the increase in both total IgG and OVA-specific IgG in OVA-immunized mice. However, no effect was observed on Ab affinity maturation . Accumulation of germinal center (GC) and memory B cells was observed in the spleens together with elevated percentages of plasma cells in the spleens and bone marrow . More interestingly, dramatic infiltration of CD4 + T cells was apparent in GCs after PD-1 blockade with a significant increase in the expression of ICOS . When CD4 + T cells and B cells from OVA-immunized mice were co-cultured with neutralizing anti-PD-1 Ab in vitro, PD-1 blockade recapitulated the up-regulation of ICOS expression on CD4 + T cells with the activation of ERK signaling. Suppression of ERK activation not only reduced ICOS expression on CD4 + T cells but also attenuated IgG production upon PD-1 blockade. Taken together, PD-1 blockade enhances humoral immunity. This process partially relies on more accumulation of CD4 + T cells in GCs with the up-regulation of ICOS expression and the promotion of B cell terminal differentiation. The regulatory pattern of PD-1 blockade illustrated here provides a new mechanism of how immune checkpoint molecules regulating humoral immune responses.
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