Spatial epitranscriptomics reveals A-to-I editome specific to cancer stem cell microniches

Author:

Lee Amos C.ORCID,Lee Yongju,Choi Ahyoun,Lee Han-ByoelORCID,Shin Kyoungseob,Lee Hyunho,Kim Ji Young,Ryu Han SukORCID,Kim Hoe Suk,Ryu Seung Yeon,Lee Sangeun,Cheun Jong-Ho,Yoo Duck Kyun,Lee Sumin,Choi Hansol,Ryu Taehoon,Yeom HuiranORCID,Kim Namphil,Noh JinsungORCID,Lee YongheeORCID,Kim Inyoung,Bae Sangwook,Kim Jinhyun,Lee Wooseok,Kim Okju,Jung Yushin,Kim Changhoe,Song Seo Woo,Choi Yeongjae,Chung Junho,Kim Byung GeeORCID,Han WonshikORCID,Kwon SunghoonORCID

Abstract

AbstractEpitranscriptomic features, such as single-base RNA editing, are sources of transcript diversity in cancer, but little is understood in terms of their spatial context in the tumour microenvironment. Here, we introduce spatial-histopathological examination-linked epitranscriptomics converged to transcriptomics with sequencing (Select-seq), which isolates regions of interest from immunofluorescence-stained tissue and obtains transcriptomic and epitranscriptomic data. With Select-seq, we analyse the cancer stem cell-like microniches in relation to the tumour microenvironment of triple-negative breast cancer patients. We identify alternative splice variants, perform complementarity-determining region analysis of infiltrating T cells and B cells, and assess adenosine-to-inosine base editing in tumour tissue sections. Especially, in triple-negative breast cancer microniches, adenosine-to-inosine editome specific to different microniche groups is identified.

Funder

National Research Foundation of Korea

Ministry of Education

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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