Humoral IgG1 responses to tumor antigens underpin clinical outcomes in immune checkpoint blockade
Summary
Tumor-infiltrating T cells have been the primary focus of cancer immunotherapy; however, accumulating evidence points to a critical role for B cells and plasma cells in shaping responses to immune checkpoint blockade. In this study, we investigated the humoral immune response in 38 patients with hepatocellular carcinoma treated with neoadjuvant anti-programmed cell death protein 1 (PD-1) therapy. In responders, defined by more than 50% tumor necrosis, we observed on-treatment enrichment of
Content
# Humoral IgG1 responses to tumor antigens underpin clinical outcomes in immune checkpoint blockade
*Published: 2026 Mar*
Tumor-infiltrating T cells have been the primary focus of cancer immunotherapy;
however, accumulating evidence points to a critical role for B cells and plasma
cells in shaping responses to immune checkpoint blockade. In this study, we
investigated the humoral immune response in 38 patients with hepatocellular
carcinoma treated with neoadjuvant anti-programmed cell death protein 1 (PD-1)
therapy. In responders, defined by more than 50% tumor necrosis, we observed
on-treatment enrichment of clonally expanded IgG1+ plasma cells within the
tumor. Clonal tracking revealed that anti-PD-1 treatment expanded preexisting B
cell clones associated with favorable clinical outcomes. Moreover, serum from
responders contained IgG1 antibodies specific to cancer/testis antigens,
including NY-ESO-1, and these humoral responses were linked to tumor-reactive T
cell activity. We independently validated these findings across seven additional
cohorts, encompassing single-cell and bulk sequencing data from 500 patients,
spatial transcriptomics from seven patients and survival analyses from 1,582
patients. Our findings apply to recently approved treatments, such as PD-1 and
vascular endothelial growth factor A (VEGF-A) blockade, but not to chemotherapy
alone, suggesting broad relevance to individuals treated with immunotherapy.
Collectively, our results demonstrate that PD-1 blockade induces tumor-specific
IgG1+ plasma cell responses that complement cellular immunity and contribute to
clinical benefit, underscoring a coordinated humoral-cellular axis in effective
antitumor immunity.
DOI: 10.1038/s41591-025-04177-6