内质网应激在阿霉素引起的心肌损伤中作用的研究进展被引量：1

Progress in the Study of Endoplasmic Reticulum Stress in Myocardial Injury Induced by Doxorubicin

下载PDF

导出

摘要阿霉素是一种广谱抗肿瘤抗生素,但是由于剂量依赖性心脏毒性作用而引起阿霉素心肌病,致其使用受到限制.阿霉素心肌病的发病机制目前了解的仍不透彻,从近几年的研究来看,普遍认为其与心肌细胞凋亡机制相关.在众多凋亡发生机制中,作为一条新的细胞凋亡信号转导通路——内质网应激反应参与并介导凋亡的发生,为阿霉素心肌病的发生发展提供了新思路.本文通过对内质网应激在阿霉素心肌病中的作用机制和最新进展进行综述,为临床的研究提供理论依据. Doxorubicin is a broad-spectrum anti-tumor antibiotic.The use of doxorubicin was limited due to dose-de-pendent cardiotoxicity,which leads to cardiomyopathy.The pathogenesis of doxorubicin cardiomyopathy is still poorly understood.Some evidences suggest that it is related to apoptosis of cardiomyocytes.The endoplasmic reticulum stress signal pathway mediates ap-optosis,which provides a new idea for the pathogenesis of doxorubicin cardiomyopathy.This paper summarizes the recent progress of endoplasmic reticulum stress in doxorubicin-induced cardiomyopathy.

作者姜蒙蒙赵婷李旭韩哲崔佳乐 Jiang Mengmeng;Zhao Ting;Li Xu;Han Zhe;Cui Jiayue(Nomian Bethune Health Science Center,Jilin University,Changchun 130021,China;Department of Physiology,School of Basic Medical Sciences,Jilin University,Changchun 130021,China;Department of Pharmacy,the First Hospital,Jilin University,Changchun 130021,China;Department of Histology and Embryology,School of Basic Medical Sciences,Jilin University,Changchun 130021,China)

机构地区吉林大学白求恩医学部吉林大学白求恩医学部基础医学院生理学系吉林大学第一医院药学部吉林大学白求恩医学部基础医学院组织学与胚胎学系

出处《国际老年医学杂志》 2019年第6期381-384,共4页 International Journal of Geriatrics

基金吉林省国际科技合作项目(20190701069GH)。

关键词阿霉素内质网应激心肌损伤细胞凋亡 Doxorubicin Endoplasmic reticulum stress Myocardial injury Cell apoptosis

分类号 R73 [医药卫生—肿瘤]

引文网络
相关文献

参考文献5

1耿娜娜,李学英,郑翔,杨蕾,吴明松.Brefeldin A调控ATF6通路增强顺铂抑制肺癌细胞增殖的作用[J].遵义医学院学报,2018,41(4):431-436. 被引量：5
2贺智慧,邵立群,宣丽颖,王春贵,魏成喜,王羽,赵明.黄芪注射液对阿霉素性心肌细胞凋亡、内质网应激与缝隙连接蛋白表达的影响[J].中国应用生理学杂志,2018,34(2):159-163. 被引量：11
3史为博,易善勇,王贺,牛世霸,王松军,李英敏,丛斌.内质网应激PERK-ATF4-CHOP信号通路参与慢性应激大鼠下丘脑神经细胞损伤[J].解剖学杂志,2018,41(3):280-284. 被引量：11
4Miao YU,Zhi-hui HE,Li-ying XUAN,Xiao-tong SHAN,Jie LONG,Jing-yi FENG,Yu WANG,Ming ZHAO.Effect of creatine phosphate sodium on miRNA378,miRNA378＊ and calumenin mRNA in adriamycin-injured cardiomyocytes[J].中国应用生理学杂志,2016,32(6):514-518. 被引量：4
5吴明松,郑翔,耿娜娜,张志敏,赵彦禹,王哲,李学英.布雷菲德菌素A通过激活IRE1-XBP1信号通路增强顺铂诱导的人肺癌GLC-82细胞凋亡[J].中国生物化学与分子生物学报,2016,32(6):672-677. 被引量：5

二级参考文献45

1苟强,王莹,关佳宁,林嘉明,姜海燕,李欣然,申凤鸽,冯嘉轩,王新辉,曲海娥,江倩,张巧灵,刘波,姜秀云.小鼠感染旋毛虫后肠道内质网应激IRE1分子通路主要基因的表达变化[J].中国兽医学报,2015,35(2):247-251. 被引量：2
2姚丽梅,陈宇明,尹瑞兴.生长激素对大鼠阿霉素心肌病心肌细胞凋亡及P_(53)的影响[J].岭南心血管病杂志,2005,11(2):137-139. 被引量：7
3Korennykh AV,Korostelev AA,Egea PF,et al.Structural and functional basis for RNA cleavage by Ire1[J].BMC Biol,2011,9:47. 被引量：1
4Rubio C,Pincus D,Korennykh A,et al.Homeostatic adaptation to endoplasmic reticulum stress depends on Ire1 kinase activity[J].J Cell Biol,2011,193(1):171-184. 被引量：1
5Ming J,Ruan S,Wang M,et al.A novel chemical,STF-083010,reverses tamoxifen-related drugresistance in breast cancer by inhibiting IRE1/XBP1[J].Oncotarget,2015,6(38):40692- 40703. 被引量：1
6Sun H,Lin DC,Guo X,et al.Inhibition of IRE1α-driven pro-survival pathways is a promising therapeutic application in acute myeloid leukemia[J].Oncotarget,2016,7(14):18735-18749. 被引量：1
7Zhou T,Lv X,Guo X,et al.RACK1 modulates apoptosis induced by sorafenib in HCC cells by interfering with the IRE1/XBP1 axis.Oncol Rep,2015,33(6):3006-3014. 被引量：1
8Kennedy D,Samali A,J?ger R.Methods for Studying ER Stress and UPR Markers in Human Cells[J].Methods Mol Biol.2015,1292:3-18. 被引量：1
9Gardner BM,Walter P.Unfolded proteins are Ire1-activating ligands that directly induce the unfolded protein response[J].Science,2011,333(6051):1891-1894. 被引量：1
10Gou Q,Wang Y,Guan JN,et al.Alternation of IREl pathway genes expression in intestine of mouse infected with parasiteTrichina spiralis[J].Chin J Vet Sci,2015,35(2):247-252. 被引量：1