Spatial maps of T cell receptors and transcriptomes reveal distinct immune niches and interactions in the adaptive immune response

细胞受体和转录组的空间图谱揭示了适应性免疫反应中不同的免疫生态位和相互作用

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作者:Sophia Liu, J Bryan Iorgulescu, Shuqiang Li, Mehdi Borji, Irving A Barrera-Lopez, Vignesh Shanmugam, Haoxiang Lyu, Julia W Morriss, Zoe N Garcia, Evan Murray, David A Reardon, Charles H Yoon, David A Braun, Kenneth J Livak, Catherine J Wu, Fei Chen3

Abstract

T cells mediate antigen-specific immune responses to disease through the specificity and diversity of their clonotypic T cell receptors (TCRs). Determining the spatial distributions of T cell clonotypes in tissues is essential to understanding T cell behavior, but spatial sequencing methods remain unable to profile the TCR repertoire. Here, we developed Slide-TCR-seq, a 10-μm-resolution method, to sequence whole transcriptomes and TCRs within intact tissues. We confirmed the ability of Slide-TCR-seq to map the characteristic locations of T cells and their receptors in mouse spleen. In human lymphoid germinal centers, we identified spatially distinct TCR repertoires. Profiling T cells in renal cell carcinoma and melanoma specimens revealed heterogeneous immune responses: T cell states and infiltration differed intra- and inter-clonally, and adjacent tumor and immune cells exhibited distinct gene expression. Altogether, our method yields insights into the spatial relationships between clonality, neighboring cell types, and gene expression that drive T cell responses.

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