Spatial transcriptomics of T and B cell receptors uncovers lymphocyte clonal dynamics in human tissue.

biorxiv(2022)

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摘要
The spatial distribution of lymphocyte clones within tissues is critical to their development, selection, and expansion. We have developed Spatial Transcriptomics of VDJ sequences (Spatial VDJ), which maps immunoglobulin and TR antigen receptors in human tissue sections. Spatial VDJ captures lymphocyte clones matching canonical T, B, and plasma cell distributions in tissues and amplifies clonal sequences confirmed by orthogonal methods. We confirm spatial congruency between paired receptor chains, develop a computational framework to predict receptor pairs, and link the expansion of distinct B cell clones to different tumor-associated gene expression programs. Spatial VDJ delineates B cell clonal diversity, class switch recombination, and lineage trajectories within their spatial context. Taken together, Spatial VDJ captures lymphocyte spatial clonal architecture across tissues, which could have important therapeutic implications. ### Competing Interest Statement CE, KT, QL, AA, HT, SS, JMo, JLu, and JF are scientific consultants for 10x Genomics Inc, which holds IP rights to the spatial technology. The remaining authors declare no competing interests.
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