1、重症感染心肌(xnj)损伤:受体阻滞剂的评价安庆市立医院(yyun)重症医学科方长太第一页,共四十一页。主要(zhyo)内容一、基本概念;二、SIC流行病学;三、SIC的临床表现;四、SIC的发病(f bng)机制;五、受体阻滞剂在SIC运用中的效果评价;六、小结第二页,共四十一页。一、基本(jbn)慨念脓毒症:感染+全身炎症反应综合征严重脓毒症:脓毒症+组织低灌注(gunzh)/脏器功能不全脓毒症休克:脓毒症+容量复苏不能纠正的休克脓毒性心肌病 Sepsis-induced cardiomyopathy(SIC):脓毒症+心肌损伤伴或不伴有心输出量减少第三页,共四十一页。主要(zhyo)内容
2、一、基本概念;二、SIC流行病学;三、SIC的临床表现;四、SIC的发病(f bng)机制;五、受体阻滞剂在SIC运用中的效果评价;六、小结第四页,共四十一页。二、SIC流行病学(li xn bn xu)The heart is one of the most frequently affected organs in sepsis.Approximately 50%of the patients who are diagnosed with sepsis exhibit signs of myocardial dysfunction.Several reports have suggeste
3、d that patients with sepsis who develop myocardial dysfunction are more likely to die compared with those without evidence of myocardial dysfunction.心脏是脓毒血症患者最常受累的器官之一,大约有50%的脓毒症患者有心功能障碍,且患有心功能障碍(zhng i)的患者其病死率明显高于无心功能障碍(zhng i)的患者。Charpentier J,Luyt CE,Fulla Y,:Brain natriuretic peptide:a marker of
4、 myocardial dysfunction and prognosis during severe sepsis.Crit Care Med32(3):660Y665,2004.Blanco J:Incidence,organ dysfunction and mortality in severe sepsis:a Spanish multicentre study.Crit Care12(6):R158,2008第五页,共四十一页。主要(zhyo)内容一、基本概念;二、SIC流行病学;三、SIC的临床表现;四、SIC的发病机制;五、受体阻滞剂在SIC运用中的效果(xiogu)评价;六、小
5、结第六页,共四十一页。三、SIC的临床表现1.急性(jxng)发生的可逆性心肌抑制 Bouhemad*等指出,左心射血分数(LVEF)可以在几天内恢复正常;2.左心收缩、舒张功能的障碍 左心室顺应性下降引起左心收缩功能降低18-60%,舒张功能降低约20%;3.右室射血分数减少 当合并ARDS时引起的肺动脉阻力增加,导致了右心室后负荷增加,进一步造成右室射血分数减少。*Bouhemad B,Nicolas-Robin A,Arbelot C,et al.Acute left ventricular dilatation and shock-induced myocardial dysfunct
6、ion.Crit Care Med,2009,37:441-447.第七页,共四十一页。三、SIC的临床表现脓毒血症伴有cTnl增高和射血分数(fnsh)50 ms from the preceding NN interval;LF,low-frequency power domain;HF,high-frequency domain;VLF,very low frequency domain;LF/HF=LFdivided by HF.Not only HRV but also baroreflex sensitivity(BRS)and chemoreflex sensitivity(CR
7、S)are significantly compromised.这些指标,在一定程度上,反应(fnyng)了脓毒症患者心率变异性降低,自率性紊乱。-Data from Schmidt et al.2005第十一页,共四十一页。四、SIC的发病机制(jzh)-自律性紊乱Prospective observational study in 89 patients with MODS,defined as an APACHE-II scoreC20.前瞻性,观察性研究;研究对象(duxing):89名诊断为MODS患者,且APACHE-II评分20分。第十二页,共四十一页。四、SIC的发病(f bn
8、g)机制-免疫炎症失调 脓毒血症激活单核、白细胞释放各种炎性因子脓毒血症激活单核、白细胞释放各种炎性因子(包括(包括IL-1,IL-6,TNF,IL-12,IL-15 and IL-18,)和后期调节介质和后期调节介质(jizh),如巨噬细胞移动抑制因子等,如巨噬细胞移动抑制因子等Activated mononuclear cells release a broad variety of proinflammatory cytokines,including IL-1,IL-6,TNF,IL-12,IL-15 and IL-18,as well as the so-called late me
9、diators,high mobility groupbox 1 and macrophage migration inhibitory factor第十三页,共四十一页。四、SIC的发病机制(jzh)-免疫炎症失调单核细胞在心脏不同(b tn)部位分布频率(Fig 2);心脏坏死带在不同部位的分布(Fig 1)。Shock2013 Apr;39(4):329-35 第十四页,共四十一页。四、SIC的发病机制(jzh)-免疫炎症失调 同同时时,脓脓毒血症毒血症诱导诱导内皮系内皮系统统 (如(如ICAM,E-selectin,von willebrand factor,VCAM-1等)等)活化,
10、增加如活化,增加如IL,TNF等炎性等炎性细细胞因子的表达。胞因子的表达。在在脓脓毒性犬毒性犬实验实验中,中,TNF-能能使左心射血分数降低,而使用使左心射血分数降低,而使用(shyng)TNF-阻滞阻滞剂时剂时,能明,能明显显提高提高脓脓毒性休克患者的毒性休克患者的LV功功能。能。-Am J Physio1992,l263(3 Pt 2):H668-H675.-Ches1992,t101(3):810-815.第十五页,共四十一页。四、SIC的发病机制-免疫(miny)炎症失调C3、IL-6、TNF-、多巴胺、多巴酚丁胺与心脏(xnzng)循环系统(MAPCISVRILVSWI/PAOP)密
11、切相关。Immunol Invest2010;39(8):849-62第十六页,共四十一页。其次,免疫效应细胞引起的促炎性信号和抗炎的信号之间失平衡。过度的全身炎症反应可能有利于器官衰竭,过量抗炎介质的发展(fzhn),也会危及各脏器功能。*Pinsky MR:Dysregulation of the immune response in severe sepsis.Am J Med Sci 2004,328:220-229.四、SIC的发病机制(jzh)-免疫炎症失调第十七页,共四十一页。四、SIC的发病机制(jzh)-循环代谢系统 Sepsis-induced cardiac dysfun
12、ction.Cardiac performance during sepsis is impaired due to changes in the macro-and microcirculation,autonomic dysfunction,and inflammation-induced intrinsic myocardial depression.The mechanisms of myocardial depression include down-regulation of adrenergic pathways,disturbed intracellular calcium(C
13、a 2)trafficking,2)trafficking,and impaired electromechanical coupling at the myofibrillar level.Mitochondrial dysfunction seems to plays a central role in this sepsis-induced organ dysfunction.大、微循环改变,自主神经功能紊乱,炎性介导的内源性心肌抑制共同(gngtng)作用诱导肾上腺素下调,干扰Ca输送,肌原纤维受损。线粒体功能障碍起到核心作用,其抑制ATP的产生,引起心肌细胞凋亡。-Crit Care
14、 Med 2007 Vol.35,No.6第十八页,共四十一页。四、SIC的发病机制(jzh)-循环代谢系统-Effects of esmolol on systemic and pulmonary hemodynamics and on oxygenation in pigs with hypodynamic endotoxin shock.第十九页,共四十一页。四、SIC的发病(f bng)机制-儿茶酚胺系统Short-term-adrenergic stimulation with catecholamines increases cardiac contractility and he
15、art rate.However,prolonged and excess stimulation can lead to myocardial damage by calcium overload and consequent cell necrosis。短期的肾上腺素能刺激儿茶酚胺增加心肌收缩力和心脏速率(sl)。然而,长期和过量的刺激可通过钙超载和随之而来的细胞坏死引起心肌损伤。-Opie LH:Receptors and signal transduction.In:Heart Physiology:From Cell to Circulation.Fourth Edition.Opi
16、e LH(Ed).London,Lippincott Williams&Wilkins,2004,pp 186 220第二十页,共四十一页。四、SIC的发病(f bng)机制-儿茶酚胺系统 -AM J RESPIR CRIT CARE MED 1999;160:458465.第二十一页,共四十一页。四、SIC的发病机制(jzh)-儿茶酚胺系统 在皮下注射20mmol/kg儿茶酚胺类药药物后,心肌凋亡(浅灰色)和坏死(hui s)(深灰色)矩形图(左);运用异丙肾上腺素不同剂量后,心肌心肌凋亡(浅灰色)和坏死(深灰色)矩形图(右)。-J Intensive Care Med2009 Sep-Oct;24(5):293-316第二十二页,共四十一页。主要(zhyo)内容一、基本概念;二、SIC流行病学;三、SIC的临床表现;四、SIC的发病机制;五、受体阻滞剂在SIC运用中的效果(xiogu)评价;六、小结第二十三页,共四十一页。五、受体阻滞剂在SIC运用(ynyng)中的效果评价随机、双盲性小鼠试验;通过不同试验方法(fngf)检测脓毒性小鼠的存活率,血流动力学,细胞因子,炎性介质等。-