|
|
|
|
|
| The advances on the mechanisms of sepsis-induced cardiac dysfunction |
| Li Ya-min, Qiao Jian-feng, Zhang Wen-xuan, Peng Zhen-yu |
| Department of Nursing, Second Xiangya Hospital, Central South University; Xiangya Nursing School, Central South University, Changsha 410011, China |
|
|
|
|
Abstract Sepsis-induced cardiac dysfunction is a serious complication of sepsis. However, the mechanisms have not been clearly elucidated. Current studies have shown that inflammation, endothelial cells injury, oxidative stress, mitochondrial dysfunction and apoptosis play an important role in sepsis-induced cardiac dysfunction. This article will review the mechanisms of sepsis-induced cardiac dysfunction.
|
|
|
|
Corresponding Authors:
Peng Zhen-yu, E-mail: pengzhenyu1999@csu.edu.cn
|
|
|
|
| [1]Singer M, Deutschman CS, Seymour CW, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3)[J]. JAMA, 2016, 315(8):801-810.
[2]Rudiger A, Singer M. Mechanisms of sepsis-induced cardiac dysfunction[J]. Crit Care Med, 2007, 35(6):1599-1608.
[3]An R, Zhao L, Xi C, et al. Melatonin attenuates sepsis-induced cardiac dysfunction via a PI3K/Akt-dependent mechanism[J]. Basic Res Cardiol, 2016, 111(1):8.
[4]Liu YC, Yu MM, Shou ST, et al. Sepsis-Induced Cardiomyopathy:Mechanisms and Treatments[J]. Front Immunol, 2017, 8:1021.
[5]Zhong J, Hwang TC, Adams HR, et al. Reduced L-type calcium current in ventricular myocytes from endotoxemic guinea pigs[J]. Am J Physiol, 1997, 273(5 Pt 2):H2312-2324.
[6]Dong LW, Wu LL, Ji Y, et al. Impairment of the ryanodine-sensitive calcium release channels in the cardiac sarcoplasmic reticulum and its underlying mechanism during the hypodynamic phase of sepsis[J]. Shock, 2001, 16(1):33-39.
[7]Wu LL, Ji Y, Dong LW, et al. Calcium uptake by sarcoplasmic reticulum is impaired during the hypodynamic phase of sepsis in the rat heart[J]. Shock, 2001, 15(1):49-55.
[8]de Pablo R, Monserrat J, Reyes E, et al. Mortality in patients with septic shock correlates with anti-inflammatory but not proinflammatory immunomodulatory molecules[J]. J Intensive Care Med, 2011, 26(2):125-132.
[9]Chang RM, Wen LQ, Chang JX, et al. Repair of damaged intestinal mucosa in a mouse model of sepsis[J]. World J Emerg Med, 2013, 4(3):223-228.
[10]Kumar A, Thota V, Dee L, et al. Tumor necrosis factor alpha and interleukin 1beta are responsible for in vitro myocardial cell depression induced by human septic shock serum[J]. J Exp Med, 1996, 183(3):949-958.
[11]Weisensee D, Bereiter-Hahn J, Schoeppe W, et al. Effects of cytokines on the contractility of cultured cardiac myocytes[J]. Int J Immunopharmacol, 1993, 15(5):581-587.
[12]Kumar A, Brar R, Wang P, et al. Role of nitric oxide and cGMP in human septic serum-induced depression of cardiac myocyte contractility[J]. Am J Physiol, 1999, 276(1 Pt 2):R265-276.
[13]Duncan DJ, Yang Z, Hopkins PM, et al. TNF-alpha and IL-1beta increase Ca2+ leak from the sarcoplasmic reticulum and susceptibility to arrhythmia in rat ventricular myocytes[J]. Cell Calcium, 2010, 47(4):378-386.
[14]Antonucci E, Fiaccadori E, Donadello K, et al. Myocardial depression in sepsis: From pathogenesis to clinical manifestations and treatment[J]. J Crit Care, 2014, 29(4):500-511.
[15]Zhang C, Mo M, Ding W, et al. High-mobility group box 1 (HMGB1) impaired cardiac excitation-contraction coupling by enhancing the sarcoplasmic reticulum (SR) Ca(2+) leak through TLR4-ROS signaling in cardiomyocytes[J]. J Mol Cell Cardiol, 2014, 74:260-273.
[16]Coldewey SM, Rogazzo M, Collino M, et al. Inhibition of IkappaB kinase reduces the multiple organ dysfunction caused by sepsis in the mouse[J]. Dis Model Mech, 2013, 6(4):1031-1042.
[17]Kalbitz M, Fattahi F, Grailer JJ, et al. Complement-induced activation of the cardiac NLRP3 inflammasome in sepsis[J]. FASEB J, 2016, 30(12):3997-4006.
[18]Zhang W, Tao A, Lan T, et al. Carbon monoxide releasing molecule-3 improves myocardial function in mice with sepsis by inhibiting NLRP3 inflammasome activation in cardiac fibroblasts[J]. Basic Res Cardiol, 2017, 112(2):16.
[19]Yu Z, Rayile A, Zhang X, et al. Ulinastatin protects against lipopolysaccharide-induced cardiac microvascular endothelial cell dysfunction via downregulation of lncRNA MALAT1 and EZH2 in sepsis[J]. Int J Mol Med, 2017, 39(5):1269-1276.
[20]Barth E, Radermacher P, Thiemermann C, et al. Role of induciblenitric oxide synthase in the reduced responsiveness of the myocardium to catecholamines in a hyperdynamic, murine model of septic shock[J]. Crit Care Med, 2006, 34(2):307-313.
[21]Escobar DA, Botero-Quintero AM, Kautza BC, et al. Adenosine monophosphate-activated protein kinase activation protects against sepsis-induced organ injury and inflammation[J]. J Surg Res, 2015, 194(1):262-272.
[22]Zaky A, Deem S, Bendjelid K, et al. Characterization of cardiac dysfunction in sepsis: an ongoing challenge[J]. Shock, 2014, 41(1):12-24.
[23]Raeburn CD, Calkins CM, Zimmerman MA, et al. Vascular cell adhesion molecule--1 expression is obligatory for endotoxin-induced myocardial neutrophil accumulation and contractile dysfunction[J]. Surgery, 2001, 130(2):319-325.
[24]Liang Y, Li X, Zhang X, et al. Elevated levels of plasma TNF-alpha are associated with microvascular endothelial dysfunction in patients with sepsis through activating the NF-kappaB and p38 mitogen-activated protein kinase in endothelial cells[J]. Shock, 2014, 41(4):275-281.
[25]van Hinsbergh VW. Endothelium--role in regulation of coagulation and inflammation[J]. Semin Immunopathol, 2012, 34(1):93-106.
[26]Galley HF. Oxidative stress and mitochondrial dysfunction in sepsis[J]. Br J Anaesth, 2011, 107(1):57-64.
[27]Hobai IA, Buys ES, Morse JC, et al. SERCA Cys674 sulphonylation and inhibition of L-type Ca2+ influx contribute to cardiac dysfunction in endotoxemic mice, independent of cGMP synthesis[J]. Am J Physiol Heart Circ Physiol, 2013, 305(8):H1189-1200.
[28]Li L, Hu BC, Chen CQ, et al. Role of mitochondrial damage during cardiac apoptosis in septic rats[J]. Chin Med J (Engl), 2013, 126(10):1860-1866.
[29]Takasu O, Gaut JP, Watanabe E, et al. Mechanisms of Cardiac and Renal Dysfunction in Patients Dying of Sepsis[J]. Am J Respir Crit Care Med, 2013, 187(5):509-517.
[30]Cimolai MC, Alvarez S, Bode C, et al. Mitochondrial Mechanisms in Septic Cardiomyopathy[J]. Int J Mol Sci, 2015, 16(8):17763-17778.
[31]Xu C, Yi C, Wang H, et al. Mitochondrial nitric oxide synthase participates in septic shock myocardial depression by nitric oxide overproduction and mitochondrial permeability transition pore opening[J]. Shock, 2012, 37(1):110-115.
[32]Peng S, Xu J, Ruan W, et al. PPAR-gamma Activation Prevents Septic Cardiac Dysfunction via Inhibition of Apoptosis and Necroptosis[J]. Oxid Med Cell Longev, 2017, 2017:8326749.
[33]Neviere R, Fauvel H, Chopin C, et al. Caspase inhibition prevents cardiac dysfunction and heart apoptosis in a rat model of sepsis[J]. Am J Respir Crit Care Med, 2001, 163(1):218-225.
[34]Carlson DL, Willis MS, White DJ, et al. Tumor necrosis factor-alpha-induced caspase activation mediates endotoxin-related cardiac dysfunction[J]. Crit Care Med, 2005, 33(5):1021-1028.
[35]Yang Z, Liu Y, Deng W, et al. Hesperetin attenuates mitochondria-dependent apoptosis in lipopolysaccharide-induced H9C2 cardiomyocytes[J]. Mol Med Rep, 2014, 9(5):1941-1946.
[36]Zhang B, Liu Y, Zhang JS, et al. Cortistatin protects myocardium from endoplasmic reticulum stress induced apoptosis during sepsis[J]. Mol Cell Endocrinol, 2015, 406:40-48. |
|
|
|
Address: 1 North 2nd Street,
Zhongguancun, 
