Обзорная статья

Induction of metastasis, cancer stem cell phenotype, and oncogenic metabolism in cancer cells by ionizing radiation

Su Yeon LeeDepartment of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan, 609-735, KoreaEui Kyong JeongDepartment of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan, 609-735, KoreaMin Kyung JuDepartment of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan, 609-735, KoreaHyun Min JeonDepartment of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan, 609-735, KoreaMin Young KimResearch Center, Dongnam Institute of Radiological and Medical Science (DIRAMS), Pusan, 619-953, KoreaCho Hee KimDNA Identification Center, National Forensic Service, Seoul, 158-707, KoreaHye Gyeong ParkNanobiotechnology Center, Pusan National University, Pusan, 609-735, KoreaSong Iy HanThe Division of Natural Medical Sciences, College of Health Science, Chosun University, Gwangju, 501-759, KoreaHo Sung KangDepartment of Molecular Biology, College of Natural Sciences, Pusan National University, Pusan, 609-735, Korea. [email protected]

2017en

ABI

Аннотация

Radiation therapy is one of the major tools of cancer treatment, and is widely used for a variety of malignant tumours. Radiotherapy causes DNA damage directly by ionization or indirectly via the generation of reactive oxygen species (ROS), thereby destroying cancer cells. However, ionizing radiation (IR) paradoxically promotes metastasis and invasion of cancer cells by inducing the epithelial-mesenchymal transition (EMT). Metastasis is a major obstacle to successful cancer therapy, and is closely linked to the rates of morbidity and mortality of many cancers. ROS have been shown to play important roles in mediating the biological effects of IR. ROS have been implicated in IR-induced EMT, via activation of several EMT transcription factors-including Snail, HIF-1, ZEB1, and STAT3-that are activated by signalling pathways, including those of TGF-β, Wnt, Hedgehog, Notch, G-CSF, EGFR/PI3K/Akt, and MAPK. Cancer cells that undergo EMT have been shown to acquire stemness and undergo metabolic changes, although these points are debated. IR is known to induce cancer stem cell (CSC) properties, including dedifferentiation and self-renewal, and to promote oncogenic metabolism by activating these EMT-inducing pathways. Much accumulated evidence has shown that metabolic alterations in cancer cells are closely associated with the EMT and CSC phenotypes; specifically, the IR-induced oncogenic metabolism seems to be required for acquisition of the EMT and CSC phenotypes. IR can also elicit various changes in the tumour microenvironment (TME) that may affect invasion and metastasis. EMT, CSC, and oncogenic metabolism are involved in radioresistance; targeting them may improve the efficacy of radiotherapy, preventing tumour recurrence and metastasis. This study focuses on the molecular mechanisms of IR-induced EMT, CSCs, oncogenic metabolism, and alterations in the TME. We discuss how IR-induced EMT/CSC/oncogenic metabolism may promote resistance to radiotherapy; we also review efforts to develop therapeutic approaches to eliminate these IR-induced adverse effects.

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Идентификаторы

DOI: 10.1186/s12943-016-0577-4

Цитирования и источники

Цитирований: 2Использованных источников: 0

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