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Detection of cancer stem cells by EMT-specific biomarker-based peptide ligands. | LitMetric

AI Article Synopsis

  • The study explores the relationship between epithelial-mesenchymal transition (EMT) in tumors and cancer stem cells (CSCs), which contribute to drug resistance and metastasis.
  • Researchers utilized specific peptides (F7 and SP) to identify and target EMT-derived cells and CSCs in a human tongue squamous carcinoma cell model.
  • Findings revealed that these peptides can effectively penetrate tumor cells and bind to those expressing high levels of certain markers, suggesting their potential for isolating these resistant cancer subpopulations.

Article Abstract

The occurrence of epithelial-mesenchymal transition (EMT) within tumors, which enables invasion and metastasis, is linked to cancer stem cells (CSCs) with drug and radiation resistance. We used two specific peptides, F7 and SP peptides, to detect EMT derived cells or CSCs. Human tongue squamous carcinoma cell line-SAS transfected with reporter genes was generated and followed by spheroid culture. A small molecule inhibitor-Unc0642 and low-dose ionizing radiation (IR) were used for induction of EMT. Confocal microscopic imaging and fluorescence-activated cell sorting analysis were performed to evaluate the binding ability and specificity of peptides. A SAS xenograft mouse model with EMT induction was established for assessing the binding affinity of peptides. The results showed that F7 and SP peptides not only specifically penetrated into cytoplasm of SAS cells but also bound to EMT derived cells and CSCs with high nucleolin and vimentin expression. In addition, the expression of CSC marker and the binding of peptides were increased in tumors isolated from Unc0642/IR-treated groups. Our study demonstrates the potential of these peptides for detecting EMT derived cells or CSCs and might provide an alternative isolation method for these subpopulations within the tumor in the future.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8599855PMC
http://dx.doi.org/10.1038/s41598-021-01138-0DOI Listing

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