Aims: Non-small-cell lung cancer (NSCLC) is the most common clinical
lung cancer. Polymorphonuclear-myeloid derived suppressor cells
(PMN-MDSCs), which are the major population of MDSCs, are involved in
NSCLC progression. Recently, it was found that lectin-type oxidized LDL
receptor 1 (LOX-1) could identify humsn PMN-MDSCs. However, the role of
CD15+LOX-1+ PMN-MDSCs in NSCLC early diagnosis has not been revealed.
Here, we tried to confirm the application of the newly-identified
CD15+LOX-1+ PMN-MDSCs in the early diagnosis of NSCLC. Methods: Flow
cytometry (FCM) was used to detect the proportion of CD15+LOX-1+
PMN-MDSCs in the peripheral blood (PB) of healthy controls (HC) and
NSCLC patients. The correlation of CD15+LOX-1+ PMN-MDSC frequency with
levels of cytokeratin 19-fragments (CYFRA21-1), carcinoembryonic antigen
(CEA), and carbohydrate antigen 125 (CA125) was analyzed. Receiver
operating characteristic (ROC) curve was used to estimate the diagnostic
efficacy of CD15+LOX-1+ PMN-MDSCs for NSCLC. Additionally, the
association of CD15+LOX-1+ PMN-MDSC frequency with NSCLC
prognosis/recurrence after surgery was explored. Results: The proportion
of CD15+LOX-1+ PMN-MDSCs increased in PB of NSCLC patients. CD15+LOX-1+
PMN-MDSC proportion was positively correlated with levels of CEA and
CYFRA21-1. The area under the ROC curve (AUC) of PMN-MDSC percentage was
higher than CYFRA21-1, CEA and CA125. The proportion of CD15+LOX-1+
PMN-MDSCs decreased in patients after surgery. The frequency of
CD15+LOX-1+ PMN-MDSCs was lower in NSCLC patients without recurrence
compared to those with recurrence after surgery. Conclusions:
Circulating CD15+LOX-1+ PMN-MDSCs are a potential diagnostic marker for
NSCLC, and are associated with NSCLC prognosis and recurrence after
surgery.
Circulating CD15
+
LOX‐1
+
PMN‐MDSCs are a potential biomarker for the early diagnosis of non‐small cell lung cancer
