Abstract
BackgroundIt is difficult to distinguish benign pulmonary nodules (PNs) from malignant PNs by conventional examination. Therefore, novel biomarkers that can identify the nature of PNs are needed. Exosomes have recently been identified as an attractive alternative approach since tumor-specific molecules can be found in exosomes isolated from biological fluids.MethodsPlasma exosomes were extracted via the exoEasy reagent method. The major proteins from plasma exosomes in patients with PNs were identified via labelfree analysis and screened for differentially expressed proteins. A GO classification analysis and KEGG pathway analysis were performed on plasma exosomal protein from patients with benign and malignant PNs.ResultsWestern blot confirmed that protein expression of CD63 and CD9 could be detected in the exosome extract. Via a search of the human Uniprot database, 736 plasma exosome proteins from patients with PNs were detected using high-confidence peptides. There were 33 differentially expressed proteins in the benign and malignant PNs. Of these, 12 proteins were only expressed in the benign PNs group, while 9 proteins were only expressed in the malignant PNs group. We further obtained important information on signaling pathways and nodal proteins related to differential benign and malignant PNs via bioinformatic analysis methods such as GO, KEGG, and String.ConclusionsThis study provides a new perspective on the identification of novel detection strategies for benign and malignant PNs. We hope our findings can provide clues for the identification of benign and malignant PNs.
Highlights
Hundreds of thousands of patients are diagnosed with pulmonary nodules (PNs) each year, and this number is on the rise [1, 2]
The final diagnoses were made according to pathological examinations performed after each operation. 10 of the 40 patients were diagnosed with benign diseases and the rest with non-small cell lung cancer (NSCLC) according to the pathological diagnosis
Exosomes identification and characterization Representative computed tomography (CT) images and pathological images of benign and malignant PNs patients are shown in Fig. 1a and b, respectively
Summary
Hundreds of thousands of patients are diagnosed with pulmonary nodules (PNs) each year, and this number is on the rise [1, 2]. Kuang et al Clin Proteom (2019) 16:5 unique glycosylation, protein, lipid, and DNA and RNA profiles and biophysical properties [5], and extracellular vesicle heterogeneity can be defined by variation in cargo between and within each size class, as well as by variation in size [6]. These vesicles have been implicated in a number of different tumor physiological processes as rich reservoirs of tumor-specific proteins and biomarkers for cancer detection and progression. Exosomes have recently been identified as an attractive alternative approach since tumor-specific molecules can be found in exosomes isolated from biological fluids
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