Ischemic Conditioning-Mediated Myocardial Protection in Relation to Duration of Coronary Occlusion 被引量：1

Ischemic Conditioning-Mediated Myocardial Protection in Relation to Duration of Coronary Occlusion

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摘要 Background: Myocardial ischemia is a dynamic process whereby a cascade of events is initiated to stimulate transition from reversible to irreversible cellular injury. Non-pharmacologic approaches to cellular protection, such as ischemic conditioning, delay onset of cellular injury in most organs in a host of animal species;however the degree of protection is limited to rather short durations of ischemia. In the present study, we examined whether protection afforded by ischemic conditioning could be extended beyond currently established limits of coronary occlusion in an in situ animal model. Methods: Rabbits (n = 106) were exposed to 30-, 60-, 120-, 180-, 240-, or 360-min coronary occlusion followed by 180-min coronary reperfusion (i.e. non-conditioned control groups). Ischemic conditioned rabbits were pre-treated by ischemic conditioning (i.e. 2-cycles of 5-min coronary occlusion and 5-min reperfusion) prior to a prolonged period of ischemia as described above. Area at risk (AR; by fluorescent microparticles) and area of necrosis (AN;by tetrazolium staining) were quantified by planimetry. Serum troponin I levels were assessed at baseline (i.e. before experimental protocol) and at the end of the experiment. Results: Changes in heart rate and hemodyamic indices were similar for all groups regardless of duration of ischemia and regardless of treatment (i.e. non-conditioned vs. ischemic conditioned). Infarcts (as percent AR) were markedly smaller (~35%) in ischemic conditioned rabbits (vs. controls) for the 30-min coronary occlusion group. With longer durations of coronary occlusion (60-, 120-, 180-, 240-min) infarcts were smaller (~20%) in ischemic conditioned groups but protection afforded was not statistically significant. With 360-min coronary occlusion, infarct size was the same for both treatment groups. Serum troponin I levels were greater in relation to infarct size as expected but no differences were detected between treatments regardless of ischemic duration. Conclusions: Ischemic conditioning limits infarct development;however, protection is limited when the duration of ischemia is extended beyond 4 hours. These findings provide further support for the concept that ischemic conditioning can delay, but does not limit myocyte necrosis. Underlying mechanisms for cellular protection remain to be established. Background: Myocardial ischemia is a dynamic process whereby a cascade of events is initiated to stimulate transition from reversible to irreversible cellular injury. Non-pharmacologic approaches to cellular protection, such as ischemic conditioning, delay onset of cellular injury in most organs in a host of animal species;however the degree of protection is limited to rather short durations of ischemia. In the present study, we examined whether protection afforded by ischemic conditioning could be extended beyond currently established limits of coronary occlusion in an in situ animal model. Methods: Rabbits (n = 106) were exposed to 30-, 60-, 120-, 180-, 240-, or 360-min coronary occlusion followed by 180-min coronary reperfusion (i.e. non-conditioned control groups). Ischemic conditioned rabbits were pre-treated by ischemic conditioning (i.e. 2-cycles of 5-min coronary occlusion and 5-min reperfusion) prior to a prolonged period of ischemia as described above. Area at risk (AR; by fluorescent microparticles) and area of necrosis (AN;by tetrazolium staining) were quantified by planimetry. Serum troponin I levels were assessed at baseline (i.e. before experimental protocol) and at the end of the experiment. Results: Changes in heart rate and hemodyamic indices were similar for all groups regardless of duration of ischemia and regardless of treatment (i.e. non-conditioned vs. ischemic conditioned). Infarcts (as percent AR) were markedly smaller (~35%) in ischemic conditioned rabbits (vs. controls) for the 30-min coronary occlusion group. With longer durations of coronary occlusion (60-, 120-, 180-, 240-min) infarcts were smaller (~20%) in ischemic conditioned groups but protection afforded was not statistically significant. With 360-min coronary occlusion, infarct size was the same for both treatment groups. Serum troponin I levels were greater in relation to infarct size as expected but no differences were detected between treatments regardless of ischemic duration. Conclusions: Ischemic conditioning limits infarct development;however, protection is limited when the duration of ischemia is extended beyond 4 hours. These findings provide further support for the concept that ischemic conditioning can delay, but does not limit myocyte necrosis. Underlying mechanisms for cellular protection remain to be established.

作者 John G. Kingma Jr. John G. Kingma Jr.(Department of Medicine, Faculty of Medicine, Pavillon Ferdinand-Vandry, Université Laval, Québec, Canada)

机构地区 Department of Medicine

出处《World Journal of Cardiovascular Diseases》 2021年第3期210-222,共13页 心血管病（英文）

关键词 ISCHEMIA REPERFUSION Infarct Size Biomarkers Ischemic Conditioning Rab-bits Ischemia Reperfusion Infarct Size Biomarkers Ischemic Conditioning Rab-bits

分类号 R54 [医药卫生—心血管疾病]

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参考文献2

1Michael Rahbek Schmidt,Kasper Pryds,Hans Erik Btker.Novel adjunctive treatments of myocardial infarction[J].World Journal of Cardiology,2014,6(6):434-443. 被引量：10
2J. G. Kingma.Conditioning Strategies Limit Cellular Injury?[J].World Journal of Cardiovascular Diseases,2014,4(11):539-547. 被引量：2

二级参考文献12

1Joo-Yong Hahn,Young Bin Song,Eun Kyoung Kim,Cheol Woong Yu,Jang-Whan Bae,Woo-Young Chung,Seung-Hyuk Choi,Jin-Ho Choi,Jang-Ho Bae,Kyung Joo An,Jong-Seon Park,Ju Hyeon Oh,Sang-Wook Kim,Jin-Yong Hwang,Jae Kean Ryu,Hun Sik Park,Do-Sun Lim,Hyeon-Cheol Gwon.Ischemic Postconditioning During Primary Percutaneous Coronary Intervention: The Effects of Postconditioning on Myocardial Reperfusion in Patients With ST-Segment Elevation Myocardial Infarction (POST) Randomized Trial[J].Circulation.2013(17)
2Gonghuan Yang,Yu Wang,Yixin Zeng,George F Gao,Xiaofeng Liang,Maigeng Zhou,Xia Wan,Shicheng Yu,Yuhong Jiang,Mohsen Naghavi,Theo Vos,Haidong Wang,Alan D Lopez,Christopher JL Murray.Rapid health transition in China, 1990–2010: findings from the Global Burden of Disease Study 2010[J].The Lancet.2013(9882)
3Hausenloy, Derek J,Yellon, Derek M.Myocardial ischemia-reperfusion injury: a neglected therapeutic target[J].Journal of Clinical Investigation.2013(1)
4Gerd Heusch.Cardioprotection: chances and challenges of its translation to the clinic[J].The Lancet.2012
5Gerd Heusch,Judith Musiolik,Eva Kottenberg,Jürgen Peters,Heinz Jakob,Matthias Thielmann.STAT5 Activation and Cardioprotection by Remote Ischemic Preconditioning in Humans[J].Circulation Research.2012(1)
6Mehri Kadkhodaee,Behjat Seifi,Atefeh Najafi,Zahra Sedaghat.First Report of the Protective Effects of Remote Per- and Postconditioning on Ischemia/Reperfusion-Induced Renal Injury[J].Transplantation.2011(10)
7Cecil D. Hahn,Cedric Manlhiot,Michael R. Schmidt,Torsten T. Nielsen,Andrew N. Redington.Remote Ischemic Per-Conditioning: A Novel Therapy for Acute Stroke?[J].Stroke.2011(10)
8Joo-Yong Hahn,Hyun-Joong Kim,Yu Jeong Choi,Sang-Ho Jo,Hak Jin Kim,Sahng Lee,Kyoung-Ju Ahn,Young Bin Song,Jin-Ho Choi,Seung-Hyuk Choi,Young-Jin Choi,Kyung-Han Lee,Sang Hoon Lee,Hyeon-Cheol Gwon.Effects of atorvastatin pretreatment on infarct size in patients with ST-segment elevation myocardial infarction undergoing primary percutaneous coronary intervention[J].American Heart Journal.2011(6)
9Woan-Ching Jan,Cay-Huyen Chen,Pei-Shan Tsai,Chun-Jen Huang.Limb ischemic preconditioning mitigates lung injury induced by haemorrhagic shock/resuscitation in rats[J].Resuscitation.2011(6)
10赵铁刚.金融危机背景下我国房地产市场可持续性发展问题初探[J].商业经济,2011(10):8-9. 被引量：1

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2王艳玲,华琦,刘志,褚研研.晚期时相肢体缺血预适应对冠状动脉介入术患者的预后影响[J].首都医科大学学报,2015,36(3):393-398. 被引量：10
3洪叶,袁勇,曹文疆,程江,王新春.香青兰总黄酮对大鼠心肌缺血再灌注损伤诱导的自噬作用的研究[J].中国药学杂志,2016,51(11):890-895. 被引量：15
4孙凯,陈文华,张颖,李燕,安梦瑶,潘莹莹,吴艳娜,康毅,高卫真,娄建石.无创性延迟肢体缺血预适应对心肌梗死大鼠预后的影响[J].中国病理生理杂志,2017,33(1):116-122. 被引量：5
5汪永生,王连生.治疗性低温处理心肌缺血／再灌注损伤的研究进展[J].中国急救医学,2017,37(9):855-859. 被引量：3
6钟芳,李珍,赵雨,郭欢.无创肢体缺血预适应训练对冠心病择期PCI术患者心脏康复的影响[J].医学理论与实践,2019,32(1):125-127. 被引量：4
7Bo Huang,Lin-Feng Huang,Ling Zhao,Zongyue Zeng,Xi Wang,Daigui Cao,Lijuan Yang,Zhenyu Ye,Xian Chen,Bin Liu,Tong-Chuan He,Xiaozhong Wang.Microvesicles(MIVs)secreted from adipose-derived stem cells(ADSCs)contain multiple microRNAs and promote the migration and invasion of endothelial cells[J].Genes & Diseases,2020,7(2):225-234. 被引量：9
8展丽元,冯丽钦,颜焕芝,马小菊,李金莲,付雪.无创肢体缺血预适应对经桡动脉行择期PCI患者的影响[J].心血管康复医学杂志,2021,30(5):545-548. 被引量：2
9陈彬,胡雨,陶建平,马智会,曾金美,张莉莉,陈忠,王兴德,张永军.远端肢体缺血预处理对AMI患者的心肌保护作用及对远期预后的影响[J].心血管康复医学杂志,2022,31(1):19-22. 被引量：2
10John G. Kingma,Denys Simard,Jacques R. Rouleau.Impact of Acute Ischemia-Reperfusion Injury on Left Ventricular Pressure-Volume Relations in Dogs[J].World Journal of Cardiovascular Diseases,2022,12(4):236-249.

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2HAN XiaoXu,LI Lan,XIE Tian,CHEN Si,ZOU Yang,JIN Xin,LI Sheng,WANG Meng,HAN Ning,FAN GuanWei,LIU WenGuang,WANG Wei.“Ferrero-like”nanoparticles knotted injectable hydrogels to initially scavenge ROS and lastingly promote vascularization in infarcted hearts[J].Science China(Technological Sciences),2020,63(11):2435-2448. 被引量：3
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5John G. Kingma,Guylaine Sénéchal,Jacques R. Rouleau,Iris Kingma.Ischemic Tolerance in Uremic Rabbits[J].World Journal of Cardiovascular Diseases,2015,5(12):351-360.
6Timur Yagudin,Yue Zhao,Haiyu Gao,Yang Zhang,Ying Yang,Xiaofang Zhang,Wenbo Ma,Tolessa Muleta Daba,Vladimir Ishmetov,Kai Kang,Baofeng Yang,Zhenwei Pan.iASPP protects the heart from ischemia injury by inhibiting p53 expression and cardiomyocyte apoptosis[J].Acta Biochimica et Biophysica Sinica,2021,53(1):102-111. 被引量：1
7Qiang Wangn,Xiaojun He,Bin Wang,Jun Pan,Chunying Shi,Jie Li,Liudi Wang,Yannan Zhao,Jianwu Dai,Dongjin Wang.Injectable collagen scaffold promotes swine myocardial infarction recovery by long-term local retention of transplanted human umbilical cord mesenchymal stem cells[J].Science China(Life Sciences),2021,64(2):269-281. 被引量：6
8Mingchuan Shao,Changshuo Shang,Fengxiang Zhang,Zhen Xu,Wei Hu,Qingqing Lu,Ligang Gai.Selective adsorption-involved formation of NMC532/PANI microparticles with high ageing resistance and improved electrochemical performance[J].Journal of Energy Chemistry,2021,30(3):668-679. 被引量：1
9Wang Chen,Wang Xiaoreng,Tao Tianqi,Song Dandan,Wang Jianli,Wang You,Liu Xiuhua,Wu Xudong.Traditional Chinese Medicines alleviated myocardial ischemia by regulating Qi and promoting blood circulation[J].Journal of Traditional Chinese Medicine,2020,40(6):974-982. 被引量：5
10Buchhorn Reiner.Myocardial Protection with Beta Blocker Treatment in Infants with Heart Failure Due to Congenital Heart Defects and Duchenne Muscular Dystrophy[J].Open Journal of Thoracic Surgery,2020,10(4):81-88. 被引量：1

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Ischemic Conditioning-Mediated Myocardial Protection in Relation to Duration of Coronary Occlusion 被引量：1

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