Mapping antibody sequences and effector functions across spatial niches

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Curr Opin Immunol. 2026 Jul 10;102:102816. doi: 10.1016/j.coi.2026.102816. Online ahead of print.

ABSTRACT

Antibodies are fundamental to human health but can also drive pathology. Each antibody has a molecular specificity, encoded by their clonally heritable B cell receptor (BCR). Recent advances in spatial transcriptomics coupled with repertoire sequencing have enabled capturing antibody-secreting cells (ASCs) and their clonal BCR within their tissue microenvironment. However, our understanding of antibody production niches remains limited. Furthermore, where antibodies are produced can be distinct from where antibodies exert their effector function. Here, we propose a conceptual spatial framework to distinguish between ‘antibody production niches’, defined by the ASC, BCR, and niche composition, versus ‘antibody functional niches’, composed of the antibody, antigen, and effector landscape. We then examine the possibilities and challenges to map and link antibody-encoding sequences and antibody effector functions using current and emerging technologies. Combined, we argue that integrating spatial sequence data with the antibody functional context is essential to decode the architecture of antibody-mediated immunity.

PMID:42430906 | DOI:10.1016/j.coi.2026.102816

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