AI Article Synopsis

  • The study investigates the use of peptide functionalized magnetic nanoparticles (Pep@MNP) to capture circulating tumor cells (CTCs) in pancreatic ductal adenocarcinoma (PDAC), focusing on the CXCR4+ CTCs, which indicate a high risk for metastasis and early recurrence.
  • The research reveals that a significant percentage of PDAC patients have detectable CTCs in both peripheral blood (79%) and portal vein blood (77.5%), with a notable proportion being highly metastatic-prone CXCR4+ CTCs (63.3% and 67.7%, respectively).
  • The findings suggest that CTC enumeration could serve as an effective diagnostic biomarker for pancreatic cancer, with enhanced predictive capabilities related to

Article Abstract

Objective: The circulating tumor cells (CTCs) could be captured by the peptide functionalized magnetic nanoparticles (Pep@MNP) detection system in pancreatic ductal adenocarcinoma (PDAC). CTCs and the CXCR4 expression were detected to explore their clinical significance. The CXCR4+ CTCs, this is highly metastatic-prone stem cell-like subsets of CTCs (HM-CTCs), were found to be associated with the early recurrence and metastasis of PDAC.

Methods: CTCs were captured by Pep@MNP. CTCs were identified via immunofluorescence with CD45, cytokeratin antibodies, and the CXCR4 positive CTCs were assigned to be HM-CTCs.

Results: The over-expression of CXCR4 could promote the migration of pancreatic cancer cell and . In peripheral blood (PB), CTCs were detected positive in 79.0% of all patients (49/62, 9 (0-71)/2mL), among which 63.3% patients (31/49, 3 (0-23)/2mL) were HM-CTCs positive. In portal vein blood (PVB), CTCs were positive in 77.5% of patients (31/40, 10 (0-40)/2mL), and 67.7% of which (21/31, 4 (0-15)/2mL) were HM-CTCs positive CTCs enumeration could be used as diagnostic biomarker of pancreatic cancer (AUC = 0.862), and the combination of CTCs positive and CA19-9 increase shows improved diagnostic accuracy (AUC = 0.963). in addition, PVB HM-CTCs were more accurate to predict the early recurrence and liver metastasis than PB HM-CTCs (AUC 0.825 vs. 0.787 and 0.827 vs. 0.809, respectively).

Conclusions: The CTCs identified by Pep@MNP detection system could be used as diagnostic and prognostic biomarkers of PDAC patients. We identified and defined the CXCR4 over-expressed CTC subpopulation as highly metastatic-prone CTCs, which was proved to identify patients who were prone to suffering from early recurrence and metastasis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11231205PMC
http://dx.doi.org/10.3389/fonc.2024.1327280DOI Listing

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