[No authors listed]
Lung adenocarcinoma (LA) is the most commonly occurring histological type of nonâsmall cell lung cancer. Diagnosis and treatment of LA remain a major clinical challenge. In the present study, to identify early LA biomarkers, extracellular vesicles (EVs) were separated from the plasma samples from 153 patients with LA and 75 healthy controls. microRNA (miRNA) expression profiling was performed at the screening stage (5 patients with LA vs. 5 controls), followed by verification at the validation stage (40 patients with LA vs. 20 controls) using reverse transcriptionâquantitative polymerase chain reaction (RTâqPCR). The four disordered miRNAs (miRâ505â5p, miRâ486â3p, miRâ486â3p and miRâ382â3p) identified in the plasma EVs were further evaluated at the testing stage (108 patients with LA vs. 50 controls) by RTâqPCR. It was revealed that miRâ505â5p was upregulated, whereas miRâ382â3p was downregulated, in the EVs from patients with LA. Furthermore, miRâ505â5p was also upregulated in tumor tissues, compared with adjacent nonâtumor control tissues. Subsequently, the direct targets of miRâ505â5p were predicted using bioinformatics analyses, and verified by luciferase assay and immunoblotting. The present study determined that miRâ505â5p functions as an oncogene, promoting lung cancer cell proliferation and inhibiting cancer cell apoptosis via the targeting of tumor protein P53âregulated apoptosisâinducing protein 1 (TP53AIP1). Finally, it was confirmed that miRâ505â5p in plasma EVs could be delivered to lung cancer cells, inhibiting cell apoptosis and promoting cell proliferation by targeting TP53AIP1. In conclusion, the present study indicated that miRNAâ505â5p functions as an oncogene that may be used as a novel biomarker for the diagnosis and treatment of LA.
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