Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy

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Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy Publisher Pubmed

Mortezaee K¹ ; Goradel NH² ; Amini P³ ; Shabeeb D^{4, 5} ; Musa AE^{4, 6} ; Najafi M⁷ ; Farhood B⁸

Show Affiliations

1. Department of Anatomy, School of Medicine, Kurdistan University of Medical Sciences, Sanandaj, Iran
2. Department of Medical Biotechnology, School of Advanced Technologies in Medicine, Tehran University of Medical Sciences, Tehran, Iran
3. Department of Radiology, Faculty of paramedical, Tehran University of Medical Sciences, Tehran, Iran
4. Department of Medical Physics & Biomedical Engineering, School of Medicine, Tehran University of Medical Sciences, International Campus, Tehran, Iran
5. Department of Physiology, College of Medicine, University of Misan, Misan, Iraq
6. Research Center for Molecular and Cellular Imaging, Tehran University of Medical Sciences, Tehran, Iran
7. Radiology and Nuclear Medicine Department, School of Paramedical Sciences, Kermanshah University of Medical Sciences, Kermanshah, Iran
8. Department of Medical Physics and Radiology, Faculty of Paramedical Sciences, Kashan University of Medical Sciences, Kashan, Iran

Source: Current Molecular Pharmacology Published:2019

Abstract

Background: Radiotherapy is a treatment modality for cancer. For better therapeutic efficiency, it could be used in combination with surgery, chemotherapy or immunotherapy. In addition to its beneficial therapeutic effects, exposure to radiation leads to several toxic effects on normal tissues. Also, it may induce some changes in genomic expression of tumor cells, thereby increasing the resistance of tumor cells. These changes lead to the appearance of some acute reactions in irradiated organs, increased risk of carcinogenesis, and reduction in the therapeutic effect of radiotherapy. Discussion: So far, several studies have proposed different targets such as cyclooxygenase-2 (COX-2), some toll-like receptors (TLRs), mitogen-activated protein kinases (MAPKs) etc., for the amelioration of radiation toxicity and enhancing tumor response. NADPH oxidase includes five NOX and two dual oxidases (DUOX1 and DUOX2) subfamilies that through the production of superoxide and hydrogen peroxide, play key roles in oxidative stress and several signaling pathways involved in early and late effects of ionizing radiation. Chronic ROS production by NOX enzymes can induce genomic instability, thereby increasing the risk of carcinogenesis. Also, these enzymes are able to induce cell death, especially through apoptosis and senescence that may affect tissue function. ROS-derived NADPH oxidase causes apoptosis in some organs such as intestine and tongue, which mediate inflammation. Furthermore, continuous ROS production stimulates fibrosis via stimulation of fibroblast differentiation and collagen deposition. Evidence has shown that in contrast to normal tissues, the NOX system induces tumor resistance to radiotherapy through some mechanisms such as induction of hypoxia, stimulation of proliferation, and activation of macrophages. However, there are some contradictory results. Inhibition of NADPH oxidase in experimental studies has shown promising results for both normal tissue protection and tumor sensitization to ionizing radiation. Conclusion: In this article, we aimed to review the role of different subfamilies of NADPH oxidase in radiation-induced early and late normal tissue toxicities in different organs. © 2019 Bentham Science Publishers.

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Style	Citing Format
MLA	Mortezaee K, et al.. "Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy." Current Molecular Pharmacology, vol. 12, no. 1, 2019, pp. 50-60.
APA	Mortezaee K, Goradel NH, Amini P, Shabeeb D, Musa AE, Najafi M, Farhood B (2019). Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy. Current Molecular Pharmacology, 12(1), 50-60.
Chicago	Mortezaee K, Goradel NH, Amini P, Shabeeb D, Musa AE, Najafi M, Farhood B. "Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy." Current Molecular Pharmacology 12, no. 1 (2019): 50-60.
Harvard	Mortezaee K et al. (2019) 'Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy', Current Molecular Pharmacology, 12(1), pp. 50-60.
Vancouver	Mortezaee K, Goradel NH, Amini P, Shabeeb D, Musa AE, Najafi M, et al.. Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy. Current Molecular Pharmacology. 2019;12(1):50-60.
BibTex	@article{ author = {Mortezaee K and Goradel NH and Amini P and Shabeeb D and Musa AE and Najafi M and Farhood B}, title = {Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy}, journal = {Current Molecular Pharmacology}, volume = {12}, number = {1}, pages = {50-60}, year = {2019} }
RIS	TY - JOUR AU - Mortezaee K AU - Goradel NH AU - Amini P AU - Shabeeb D AU - Musa AE AU - Najafi M AU - Farhood B TI - Nadph Oxidase As a Target for Modulation of Radiation Response; Implications to Carcinogenesis and Radiotherapy JO - Current Molecular Pharmacology VL - 12 IS - 1 SP - 50 EP - 60 PY - 2019 ER -

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