| Literature DB >> 33332768 |
Hassan Massalha1, Keren Bahar Halpern1, Samir Abu-Gazala2,3, Tamar Jana1, Efi E Massasa1, Andreas E Moor4, Lisa Buchauer1, Milena Rozenberg1, Eli Pikarsky5, Ido Amit6, Gideon Zamir2, Shalev Itzkovitz1.
Abstract
Malignant cell growth is fueled by interactions between tumor cells and the stromal cells composing the tumor microenvironment. The human liver is a major site of tumors and metastases, but molecular identities and intercellular interactions of different cell types have not been resolved in these pathologies. Here, we apply single cell RNA-sequencing and spatial analysis of malignant and adjacent non-malignant liver tissues from five patients with cholangiocarcinoma or liver metastases. We find that stromal cells exhibit recurring, patient-independent expression programs, and reconstruct a ligand-receptor map that highlights recurring tumor-stroma interactions. By combining transcriptomics of laser-capture microdissected regions, we reconstruct a zonation atlas of hepatocytes in the non-malignant sites and characterize the spatial distribution of each cell type across the tumor microenvironment. Our analysis provides a resource for understanding human liver malignancies and may expose potential points of interventions.Entities:
Keywords: human cell atlas; liver cancer; single cell RNAseq; spatial transcriptomics; tumor-stroma interactions
Year: 2020 PMID: 33332768 DOI: 10.15252/msb.20209682
Source DB: PubMed Journal: Mol Syst Biol ISSN: 1744-4292 Impact factor: 11.429