吗啡在体内对大鼠心脏诱导晚期心脏保护作用:阿片受体和核转录因子κB的参与。
Morphine induces late cardioprotection in rat hearts in vivo: the involvement of opioid receptors and nuclear transcription factor kappaB.
作者信息
Frässdorf Jan, Weber Nina C, Obal Detlef, Toma Octavian, Müllenheim Jost, Kojda Georg, Preckel Benedikt, Schlack Wolfgang
机构信息
Department of Anesthesiology, University Hospital of Düsseldorf, Düsseldorf, Germany.
出版信息
Anesth Analg. 2005 Oct;101(4):934-941. doi: 10.1213/01.ane.0000172130.70274.84.
UNLABELLED
Delta1-opioid receptor agonists can induce cardioprotection by early and late preconditioning (LPC). Morphine (MO) is commonly used for pain treatment during acute coronary syndromes. We investigated whether MO can induce myocardial protection by LPC and whether a nuclear transcription factor kappaB (NF-kappaB)-dependent intracellular signaling pathway is involved. Rats were subjected to 25 min of regional ischemia and 2 h of reperfusion 24 h after treatment with saline (NaCl; 0.9% 5 mL), lipopolysaccharide of Escherichia coli (LPS; 1 mg/kg), or MO (3 mg/kg). LPS is a trigger of LPC and served as positive control. Naloxone (NAL) was used to investigate the role of opioid receptors in LPC and was given before NaCl, LPS, or MO application (trigger phase) or before ischemia-reperfusion (mediator phase). Infarct size (percentage area at risk) was 59% +/- 9%, 51% +/- 6%, or 53% +/- 10% in the NaCl, NAL-NaCl, and NaCl-NAL groups, respectively. Pretreatment with MO reduced infarct size to 20% +/- 6% after 24 h (MO-24h), and this effect was abolished by NAL in the trigger (NAL-MO, 53% +/- 14%) and in the mediator (MO-NAL, 60% +/- 8%) phases. Pretreatment with LPS reduced infarct size to 23% +/- 8%. NAL administration in the trigger phase had no effect on infarct size (NAL-LPS 30% +/- 16%), whereas NAL during the mediator phase of LPC abolished the LPS-induced cardioprotection (LPS-NAL 54% +/- 8%). The role of NF-kappaB in morphine-induced LPC was investigated by Western blot and electrophoretic mobility shift assay. Morphine and LPS treatment increased phosphorylation of the inhibitory protein kappaB, leading to an increased activity of NF-kappaB. Thus, MO induces LPC similarly to LPS and it is likely that this cardioprotection is mediated at least in part by activation of NF-kappaB. Opioid receptors are involved as mediators in both MO- and LPS-induced LPC but as triggers only in MO-induced LPC.
IMPLICATIONS
Like lipopolysaccharide, morphine induces late preconditioning and activation of nuclear transcription factor-kappaB. Opioid receptors are involved as mediators in both morphine- and lipopolysaccharide-induced late preconditioning but as triggers only in morphine-induced late preconditioning.
未标记
δ1-阿片受体激动剂可通过早期和晚期预处理(LPC)诱导心脏保护作用。吗啡(MO)常用于急性冠脉综合征期间的疼痛治疗。我们研究了MO是否能通过LPC诱导心肌保护作用,以及是否涉及核转录因子κB(NF-κB)依赖性细胞内信号通路。大鼠在接受生理盐水(NaCl;0.9% 5 mL)、大肠杆菌脂多糖(LPS;1 mg/kg)或MO(3 mg/kg)治疗24小时后,进行25分钟的局部缺血和2小时的再灌注。LPS是LPC的触发因素,用作阳性对照。纳洛酮(NAL)用于研究阿片受体在LPC中的作用,在应用NaCl、LPS或MO之前(触发阶段)或缺血-再灌注之前(介导阶段)给药。NaCl组、NAL-NaCl组和NaCl-NAL组的梗死面积(危险区域百分比)分别为59%±9%、51%±6%或53%±10%。MO预处理24小时后(MO-24h)梗死面积降至20%±6%,而在触发阶段(NAL-MO,53%±14%)和介导阶段(MO-NAL,60%±8%),NAL消除了这种作用。LPS预处理使梗死面积降至23%±8%。在触发阶段给予NAL对梗死面积无影响(NAL-LPS 30%±16%),而在LPC的介导阶段给予NAL则消除了LPS诱导的心脏保护作用(LPS-NAL 54%±8%)。通过蛋白质免疫印迹法和电泳迁移率变动分析研究了NF-κB在吗啡诱导的LPC中的作用。吗啡和LPS处理增加了抑制蛋白κB的磷酸化,导致NF-κB活性增加。因此,MO与LPS类似地诱导LPC,这种心脏保护作用可能至少部分是由NF-κB的激活介导的。阿片受体在MO和LPS诱导的LPC中均作为介导因素起作用,但仅在MO诱导的LPC中作为触发因素起作用。
启示
与脂多糖一样,吗啡可诱导晚期预处理并激活核转录因子-κB。阿片受体在吗啡和脂多糖诱导的晚期预处理中均作为介导因素起作用,但仅在吗啡诱导的晚期预处理中作为触发因素起作用。
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