Resolving the spatial and cellular architecture of lung adenocarcinoma by multi-region single-cell sequencing

Author:

Sinjab Ansam,Han Guangchun,Treekitkarnmongkol Warapen,Hara Kieko,Brennan Patrick,Dang Minghao,Hao Dapeng,Wang Ruiping,Dai Enyu,Dejima Hitoshi,Zhang Jiexin,Bogatenkova Elena,Sanchez-Espiridion Beatriz,Chang Kyle,Little Danielle R.,Bazzi Samer,Tran Linh,Krysan Kostyantyn,Behrens Carmen,Duose Dzifa,Parra Edwin R.,Raso Maria Gabriela,Solis Luisa M.,Fukuoka Junya,Zhang Jianjun,Sepesi Boris,Cascone Tina,Byers Lauren,Gibbons Don L.,Chen Jichao,Moghaddam Seyed Javad,Ostrin Edwin J.,Rosen Daniel G.,Heymach John V.,Scheet Paul,Dubinett Steven,Fujimoto Junya,Wistuba Ignacio I.,Stevenson Christopher S.,Spira Avrum E.,Wang Linghua,Kadara Humam

Abstract

ABSTRACTLittle is known of the geospatial architecture of individual cell populations in lung adenocarcinoma (LUAD) evolution. Here, we perform single-cell RNA sequencing of 186,916 cells from 5 early-stage LUADs and 14 multi-region normal lung tissues of defined spatial proximities from the tumors. We show that cellular lineages, states, and transcriptomic features geospatially evolve across normal regions to LUADs. LUADs also exhibit pronounced intratumor cell heterogeneity within single sites and transcriptional lineage-plasticity programs. T regulatory cell phenotypes are increased in normal tissues with proximity to LUAD, in contrast to diminished signatures and fractions of cytotoxic CD8+ T cells, antigen-presenting macrophages and inflammatory dendritic cells. We further find that the LUAD ligand-receptor interactome harbors increased expression of epithelial CD24 which mediates pro-tumor phenotypes. These data provide a spatial atlas of LUAD evolution, and a resource for identification of targets for its treatment.Statement of significanceThe geospatial ecosystem of the peripheral lung and early-stage LUAD is not known. Our multi-region single-cell sequencing analyses unravel cell populations, states, and phenotypes in the spatial and ecological evolution of LUAD from the lung that comprise high-potential targets for early interception.

Publisher

Cold Spring Harbor Laboratory

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