Spatial and single-cell transcriptomics decipher the cellular environment containing HLA-G+ cancer cells and SPP1+ macrophages in colorectal cancer

Yuki Ozato,Ayako Suzuki,Yuuichi Hisamatsu,Kazunari Murakami,Satoshi Nagayama,Takeharu Sakamoto,Yuichiro Doki,Yutaka Suzuki,Mitsuaki Utou,Takeshi Iwasaki,Yoshinao Oda,Satoshi Fukuchi,Koshi Mimori,Takaaki Masuda,Masaki Mori,Kiyomi Imamura,Teppei Shimamura,Masanobu Oshima,Taro Tobo,Yasuhiro Kojima,Mamoru Uemura,Yuta Kuze,Ayako Gamachi,Shuto Hayashi,Kouichi Kagawa,Atsushi Niida,Yuta Kobayashi,Eiji Oki,Tatsuhiro Shibata,Haruka Hirose,Takeo Toshima,Junko Zenkoh,Hidetoshi Eguchi,Mituko Fukunaga,Yutaka Yonemura ,Junichi Koseki ,Yasuhiro Gotô

doi:10.1016/j.celrep.2022.111929

Abstract

The cellular interactions in the tumor microenvironment of colorectal cancer (CRC) are poorly understood, hindering patient treatment. In the current study, we investigate whether events occurring at the invasion front are of particular importance for CRC treatment strategies. To this end, we analyze CRC tissues by combining spatial transcriptomics from patients with a public single-cell transcriptomic atlas to determine cell-cell interactions at the invasion front. We show that CRC cells are localized specifically at the invasion front. These cells induce human leukocyte antigen G (HLA-G) to produce secreted phosphoprotein 1 (SPP1)+ macrophages while conferring CRC cells with anti-tumor immunity, as well as proliferative and invasive properties. Taken together, these findings highlight the signaling between CRC cell populations and stromal cell populations at the cellular level.

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