AB059. Mutant KRAS cells release tumor specific exosomes that create an immunosuppressive phenotype in lung tumor microenvironment

Savvas Petanidis; Kalliopi Domvri; Zogas Nikolaos; Paul Zarogoulidis; Efrosini Kioseoglou; Doxakis Anestakis; Konstantinos Zarogoulidis; Athanasios Salifoglou

doi:10.21037/atm.2016.AB059

Abstract

AB059. Mutant KRAS cells release tumor specific exosomes that create an immunosuppressive phenotype in lung tumor microenvironment

Savvas Petanidis¹, Kalliopi Domvri², Zogas Nikolaos³, Paul Zarogoulidis², Efrosini Kioseoglou¹, Doxakis Anestakis^4,5, Konstantinos Zarogoulidis², Athanasios Salifoglou¹

¹Department of Chemical Engineering, Aristotle University of Thessaloniki, Thessaloniki, Greece;²Pulmonary Department-Oncology Unit, General Hospital “G. Papanikolaou”, Aristotle University of Thessaloniki, Thessaloniki, Greece;³Gene and Cell Therapy Center, Hematology Department-Bone Marrow Transplantation Unit, George Papanicolaou Hospital, Thessaloniki, Greece;⁴Department of Medicine, Laboratory of General Biology, ⁵Department of Medicine, Laboratory of Forensic Medicine and Toxicology, Aristotle University of Thessaloniki, Thessaloniki, Greece

Background: To investigate whether KRAS-secreted exosomal RNAs contribute to metastatic related-EMT phenotype, and their association with the hypoxic immunosuppressive phenotype in lung carcinoma.

Methods: Lung cancer patient tissues and mice were used for exosome isolation. Exosomal molecular characterization was performed using Immunofluorescence microscopy, microRNA analysis and immunohistochemistry.

Results: The findings reveal that mutant KRAS secreted exosomes contain high expression of oncogenic miR-31/miR-182/miR-205 which are associated with HIF-2a-related hypoxia. Furthermore, exosomal secretion in lung tumor microenvironment caused accumulation of IL-10, CTL-4 and IDO suggesting KRAS-dependent exosomal immunosuppression that drives EMT-related lung metastasis.

Conclusions: These findings suggest that KRAS secreted exosomal miRNAs can modulate the hypoxic immunosuppressive mechanism in lung tumor microenvironment and trigger the EMT-related metastatic niche.

Keywords: Lung cancer; KRAS; hypoxia; immunosuppression

doi: 10.21037/atm.2016.AB059

Cite this abstract as: Petanidis S, Domvri K, Nikolaos Z, Zarogoulidis P, Kioseoglou E, Anestakis D, Zarogoulidis K, Salifoglou A. Mutant KRAS cells release tumor specific exosomes that create an immunosuppressive phenotype in lung tumor microenvironment. Ann Transl Med 2016;4(22):AB059. doi: 10.21037/atm.2016.AB059

AB059. Mutant KRAS cells release tumor specific exosomes that create an immunosuppressive phenotype in lung tumor microenvironment

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