SeQuoIA: a single-cell BCR sequencing analysis pipeline for tracking selection mechanisms in germinal centres

Germinal centres (GCs) are specialized structures where B cells undergo iterative steps of B-cell receptor (BCR) somatic hypermutation and selection of best antigen binders in a darwinian-like fashion. The accelerated evolutionary process leads to the production of high-affinity antibodies that are crucial for robust and long-term humoral immunity. Within this frame, single-cell BCR sequencing analysis is a method of choice to track GC B cell dynamics as somatic mutations can be utilised as an in vivo molecular tracer. Herein, we present SeQuoIA, a start-to-finish pipeline for the analysis of BCR repertoire sequencing data at the single-cell level, including improved clonotype assignment and phylogeny reconstruction. Most importantly, we introduce a new method for the inference of BCR-driven selection pressure based on somatic mutation patterns, that was validated with biological data. With this pipeline, we explored public datasets and proposed new selection mechanisms in GCs.