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Journal Of Modern Oncology[ISSN:1672-4992/CN:61-1415/R]

Issue:

2018 06

Page:

968-971

Research Field:

Publishing date:

Info

Title:

The sonodynamic therapy mediated reactive oxygen species and the research progress of tumor

Author(s):

Song Dan; Li Donghan; Wang Liyuan; Yue Qi

Department of Gynaecology and Obstetrics,Fourth Hospital of Harbin Medical University,Heilongjiang Harbin 150000,China.

Keywords:

sonodynamic therapy; reactive oxygen species; cancer cells

PACS:

R730.58

DOI:

10.3969/j.issn.1672-4992.2018.06.039

Abstract:

Sonodynamic therapy has been paid attention by scholars,because of its small injury,the selective and higher characteristics of the tumor treatment.Current research found,sonodynamic therapy has many mechanisms,and free radical ion theory was considered to be the main mechanism,which theory was mainly concerned with reactive oxygen species.ROS is a research hotspot in various medical fields in recent years.Oxidative stress caused the production of reactive oxygen,which has a different effect on the body.Oxidative stress and has close connection with the occurrence and development of tumor,in the role of a variety of carcinogenic factors,the body will produce a large number of ROS,if the body not to produce reactive oxygen species to clear in time,it may cause damage to the surrounding tissues,appear even malignant.This paper describes the relationship between ROS and tumor produced under the action of SDT,in order to provide new ideas for the treatment and prevention of tumors in clinic.

References:

［1］Umemura S,Yumita N,Nishigaki R.Mechanism of cell damage by ultrasound in combination with hematoporphyrin［J］.Jpn J Cancer Res,1990,81(9):962-966.
［2］McHale AP,Callan JF,Nomikou N,et al.Sonodynamic therapy：Concept,mechanism and application to cancer treatment［J］.Adv Exp Med Biol,2016,880:429-450.
［3］Costley D,Mc Ewan C,Fowley C,et al.Treating cancer with sonodynamic therapy:A review［J］.Int J Hyperthermia,2015,31(2):107-117.
［4］Li YM,Han FJ,Yin S,et al.The current study of sonodynamic therapy［J］.Cancer Research and Clinic,2015,27(3):204-206.［李艳梅,韩福军,阴爽,等.声动力学疗法的现况研究［J］.肿瘤研究与临床,2015,27(3):204-206.］
［5］Su X,Wang P,Yang S.Sonodynamic therapy induces the interplay between apoptosis and autophagy in K562 cells throught ROS［J］.Int J Biochem Biol,2015,60:82-92.
［6］Liu X,Li W,Geng S.Apoptosis induced by sonodynamic therapy in human osteosarcoma cell in vitro［J］.Mol Med Rep,2015,12(1):1183-1188.
［7］Ling Longfei,Li Yanjing,Bai Yuxian.The research progress of sonodynamic therapy on the mechanism of tumor cells［J］.Modern Oncology,2015,23(08):1142-1144.［凌龙飞,李燕京,白玉贤.声动力疗法对肿瘤细胞作用机制的研究进展［J］.现代肿瘤医学,2015,23(08):1142-1144.］
［8］Jia Dexin,Du Xiaoxue,Li Yanjing,et al.The development of sonodynamic therapy in tumor［J］.Modern Oncology,2016,24(01):152-154.［贾德馨,杜晓雪,李燕京,等.声动力疗法在肿瘤中的研究进展［J］.现代肿瘤医学,2016,24(01):152-154.］
［9］Xiang JY,Xia XS,Jiang Y,et al.Apoptosis of ovarian cancer cellsinduced bymethylene blue-mediated sonodynamic action［J］.Ultrasonics,2011,51(3):390-395．
［10］Chang J,Sun X,Guo S,et al.Effects of 5-aminolevulinic acid-mediated sonodynamietherapyon macrophages［J］.Int J Nanomedicine,2013,8:669-676．
［11］Calzavara-Pinton P,Rossi MT,Sala R,et al.Photodynamic antifungal chemotherapy［J］.Photochemistry & Photobiology,2012,88(3):512-522.
［12］Manisova B,Binder S,Malina L,et al.Phthalocyanine-mediated Photodynamic treatment of tumoural and non-tumoural cell lines［J］.Anticancer Res,2015,35(7)：3943-3951．
［13］Nyman ES,Hynninen PH.Research advances in the use oftetrapyrrolic photosensitizers for photodynamic therapy［J］.J Photochem Photobiol B,2004,73(1／2):1-28．
［14］Wan GY,Liu Y,Chen BW,et al.Recent advances of sonodynamic therapy in cancer treatment［J］.Cancer Biol Med,2016,13(3):325-338.
［15］ Li JH,Yue W,Huang Z,et al.Calcium overload induces C6 rat glioma cell apoptosis in sonodynamictherapy［J］.Int J Radiat Biol,2011,87(10):1061-1066.
［16］Dai HS,Hu SS,Wu CJ.Apoptotic effect of sonodynamic therapymediated by hematoporphyrin monomethyl ether on C6 glioma cells in vitro［J］.Acta Neurochir,2009,151:1655-1661.
［17］Sun HZ,Ge WJ,Gao X,et al.Apoptosis-promoting effects of hematoporphyrin monomethyl ether-sonodynamic therapy(HMME-SDT) on endometrial cancer［J］.Plos One,2015,10(9):e0137980.
［18］Yi LR,Zhang CL.Care during ultrasound combining with hemoporphgrin therapy for liver Cancer［J］.Acta Academiae Medicinae CPAPF,2002,11(2):116.［伊兰茹,张春丽.超声血卟啉治疗肝癌的护理［J］.武警后勤学院学报(医学版),2002,11(2):116.］
［19］Handy DE,Loscalzo J.Redox regulation of mitochondrial function［J］.Antioxid Redox Signal,2012,16(11):1323-1367.
［20］Donaghy L,Hong HK,Jauzein C,et al.The known andunknown sources of reactive oxygen and nitrogen species inhaemocytes of marine bivalve mollusks［J］.Fish&Shellfish Immunology,2015,42(1):91-97.
［21］ Mittal M,Siddiqui MR,Tran K,et al.Reactiveoxygen species in infl ammation and tissue injury［J］.Antioxidants Redox Signaling,2014,20(7):1126-1167.
［22］Sun SY,Han R.Reactive oxygen and tumor occur［J］.Foreign Medicine Oncology Branch,1990,17(2):65-68.［孙士勇,韩锐.活性氧与肿瘤发生［J］.国外医学·肿瘤学分册,1990,17(2):65-68.］
［23］Wang L,Azad N,Kongkaneramit L,et al.The fas death signaling pathway connectingreacdveoxygen speciesgeneration and FLICEinhibitory protein down-regulation［J］．The Journal of lmmunology,2008,180(5):3072-3080．
［24］Liu WH,Chang LS.Araehidonic acid induces Fas and FasL upregulation in human leukemia U937 ceils via Ca2+/ROS-Mediated suppression of ERK/e-Fos pathwayand activation of p38 MAP/ATF-2 pathway［J］.Toxicology Letters,2009,191(2-3):140-148．
［25］Cox AG,Pullar JM,Hughes G,et al.Oxidation of mitochondrialperoxiredoxin 3 during the initiation of receptor-mediated apoptosis［J］.Free Radical Biology Medicine,2008,44(6):1001-1009．
［26］Ozben T.Oxidative stress and apoptosis:Impact on cancer therapy［J］.Journal of Pharmaceutical Sciencess,2007,96(9):2181-2196．
［27］Park YH,Kim SU,Lee BK,et al.Prx I suppressesK-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/cyclin D1 pathway［J］.Antioxid Redox Signal,2013,19(5):482-496.
［28］Allen RG,Balin AK.Oxidative influnce on development and differentiation:An overview of a free radical theory of development［J］.Free Radical Biology & Medicine,1989,6(6):631-661.
［29］ Wang J,Yi J.Cancer cell killingvia ROS:To increase or decrease,that is a question［J］.Cancer Biol Ther,2008,7(12):1875-1884.
［30］Wang Y,Yang J,Yi J,Redox sensing by proteins:Oxidative modifications on cysteines and the consequent events［J］.Antioxidants & Redox Signaling,2012,16(7):649-657.
［31］Wu TT,Lu CL,Lin HI,et al.β-elemonic acidinhibits the cell proliferation of human lung adenocarcinoma A549 cells:The role of MAPK,ROS activation and glutathione depletion［J］.Oncology Rep,2016,35(1):227-234.
［32］Ni CH,Yu CS,Lu HF,et al.Chrysophanol-induced cell death(necrosis) in human lung cancer A549 cells is mediated through increasing reactive oxygenspecies and decreasing the level of mitochondrial membrane potential［J］.Environ Toxicol,2014,29(7):740-749.
［33］Pallichankandy S,Rahman A,Thayyullathil F,et al.ROS-dependent activation of autophagy is a critical mechanism for theinduction of anti-glioma effect of sanguinarine［J］.Free Radical Biology and Medicine,2015,89:708-720.
［34］Pavlova NN,Thompson CB.The emerging hallmarks of cancer metabolism［J］.Cell Metab，2016,23(1):27-47．
［35］Kobashigawa S,Kashino G,Suzuki K,et al.Ionizing radiation-induced cell death is partly caused by increase of mitochondrial reactive oxygen species in normal human fibroblast cells［J］.Radiat Res,2015,183(4):455-464．
［36］Hass C,Belz K,Schoeneberger H,et al.Sensitization of acute lymphoblastic leukemia cells for lcl161-induced cell death by targeting redox homeostasis［J］.Biochem Pharmacol,2016,105:14-22．
［37］Porporato PE,Payen VL,Perez-Escuredo J,et al.A mitochondrial switch promotes tumor metastasis［J］.Cell Rep,2014,8(3):754-766．
［38］Kim Y,Jeong IG,You D,et al.Sodium meta-arsenite induces reactive oxygen species-dependent apoptosis,necrosis,and autophagy in both androgen-sensitiveand androgen-insensitive prostate cancer cells［J］.Anti-Cancer Drug,2014,25(1):53-62.
［39］Mustafa EH,Mahmoud HT,Al-Hudhud MY,et al.2-deoxy-D-glucose synergizes with doxorubicin or L-buthionine sulfoximine to reduce adhesion and migration of breast cancer cells［J］.Asian Pac J Cancer P,2015,16(8):3213-3222.
［40］Tekiner-Gulbas B,Westwell AD,Suzen S.Oxidative stress incarcinogenesis:New synthetic compounds with dual effects uponfree radicals and cancer［J］.Curr Med Chem,2013,20(36):4451-4459.
［41］Guabiraba R,Campanha-Rodrigues AL,Souza A,et al.The flavonoid dioclein reduces the production of pro-inflammatory mediators in vitro byinhibiting PDE4 activity and scavenging reactive oxygen species［J］.Eur J Pharmacol,2010,633(1/2/3):85-92.
［42］SunY,Pu LY,Lu L,et al.N-acetylcysteineattenuates reactive-oxygen-species-mediated endoplasmicreticulum stress during liver ischemia-reperfusion injury［J］.World J Gastroenterol,2014,20(41):15289-15298.

Memo

Memo:

哈尔滨市科技局优秀学科带头人项目（编号： 2014RFXGJ035）

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Last Update: 2018-01-29