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Accession of Tumor Heterogeneity by Multiplex Transcriptome Profiling of Single Circulating Tumor Cells
[摘要] BACKGROUND: Transcriptome analysis of circulating tumor cells (CTCs) holds great promise to unravel the biology of cancer cell dissemination and identify expressed genes and signaling pathways relevant to therapeutic interventions.METHODS: CTCs were enriched based on their EpCAM expression (CellSearch®) or by size and deformability (ParsortixTM), identified by EpCAM and/or pan-keratin–specific antibodies, and isolated for single cell multiplex RNA profiling.RESULTS: Distinct breast and prostate CTC expression signatures could be discriminated from RNA profiles of leukocytes. Some CTCs positive for epithelial transcripts ( EpCAM and KRT19 ) also coexpressed leukocyte/mesenchymal associated markers ( PTPRC and VIM ). Additional subsets of CTCs within individual patients were characterized by divergent expression of genes involved in epithelial–mesenchymal transition (e.g., CDH2 , MMPs , VIM , or ZEB1 and 2 ), DNA repair ( RAD51 ), resistance to cancer therapy (e.g., AR , AR-V7, ERBB2, EGFR ), cancer stemness (e.g., CD24 and CD44 ), activated signaling pathways involved in tumor progression (e.g., PIK3CA and MTOR ) or cross talks between tumors and immune cells (e.g., CCL4 , CXCL2 , CXCL9 , IL15 , IL1B , or IL8 ).CONCLUSIONS: Multimarker RNA profiling of single CTCs reveals distinct CTC subsets and provides important insights into gene regulatory networks relevant for cancer progression and therapy.
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[效力级别]  [学科分类] 过敏症与临床免疫学
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