[血管活性肠肽对脂多糖诱导大鼠急性肺损伤中Toll样受体(TLR)2 mRNA和TLR4 mRNA表达的影响]
[Effects of vasoactive intestinal peptide on Toll-like receptor (TLR) 2 mRNA and TLR4 mRNA expression on acute lung injury induced by lipopolysaccharide in rat].
作者信息
Zuo Wen-qiong, Zhang Yu-cai, Gong Xiao-hui, Zhang Yu-ming
机构信息
Pediatric Institute for Critical Illness Research, Critical Care Center of Children's Hospital Affiliated to Shanghai Jiao tong University, Shanghai 200040, China.
出版信息
Zhonghua Er Ke Za Zhi. 2010 Jan;48(1):19-23.
OBJECTIVE
Vasoactive intestinal peptide (VIP) is a neuro-peptide that can modulate immunity. Previous studies indicated that VIP can attenuate the deleterious consequences of severe sepsis and septic shock by regulating production of inflammatory cytokines in immune activated cells. The signaling induced by bacterial components occurs primarily through Toll like receptors (TLRs). TLRs have been recognized to play a key role in pathogen recognition and innate immunity. It was convincingly demonstrated that lung is one of early suffered disaster organ and may trigger multiple organ dysfunction syndrome in sepsis. The present study was conducted to investigate the effects of VIP on TLR2/4 mRNA expressions on acute lung injury of endotoxic shock induced by lipopolysaccharide (LPS) in rat.
METHOD
Forty Sprague-Dawley rats were randomly divided into 3 groups, i.e., LPS shock group (n = 16), LPS + VIP group (n = 16), and control group (n = 8). LPS shock model was established by LPS (E. coli O(55)B(5) 10 mg/kg) with tail intravenous injection. The rats in LPS + VIP group were given a bolus of 5 nmol VIP intravenous injection follow by LPS. The rats in control group were given normal saline. The rats were sacrificed at 6 h, 24 h after being injected. The lung tissues were collected. The TLR2 mRNA and TLR4 mRNA expressions were detected by RT-PCR from the lung tissues. Pathological changes of the lungs were observed by light microscope and electron microscope 24 h after LPS injection.
RESULT
(1) Lung histopathology: the alveolar space was full with leukocyte, necrotic cells, segmental hemorrhage and protein effusion. Partial alveolar space was enlarged, lung interstitial edema were observed in LPS shock group. However, pathological changes of LPS + VIP group were milder than those in LPS shock group. (2) The expressions of TLR2 mRNA and TLR4 mRNA were significantly higher in LPS shock group compared with those of the control group (F = 16.638, P = 0.000; t = 5.876, P = 0.000), TLR2 mRNA and TLR4 mRNA expression on 24 h was down-regulated in LPS + VIP shock subgroup than those in LPS shock subgroup (F = 16.676, P = 0.000; t = 3.946, P < 0.001).
CONCLUSION
Expressions of TLR2 mRNA and TLR4 mRNA were up-regulated on LPS induced lung injury in rats. VIP mitigated lung injury induced by LPS, which may be related to TLR2 mRNA and TLR4 mRNA down-regulation of expression. The effect of VIP may suggest a protective mechanism in sepsis. VIP may play a potential protective role in severe infection.
目的
血管活性肠肽(VIP)是一种可调节免疫的神经肽。既往研究表明,VIP可通过调节免疫激活细胞中炎性细胞因子的产生,减轻严重脓毒症和脓毒性休克的有害后果。细菌成分诱导的信号传导主要通过Toll样受体(TLR)发生。TLR已被认为在病原体识别和固有免疫中起关键作用。有充分证据表明,肺是脓毒症早期受累的器官之一,可能引发多器官功能障碍综合征。本研究旨在探讨VIP对内毒素休克诱导的大鼠急性肺损伤中TLR2/4 mRNA表达的影响。
方法
40只Sprague-Dawley大鼠随机分为3组,即脂多糖(LPS)休克组(n = 16)、LPS + VIP组(n = 16)和对照组(n = 8)。通过尾静脉注射LPS(大肠杆菌O(55)B(5) 10 mg/kg)建立LPS休克模型。LPS + VIP组大鼠在注射LPS后静脉推注5 nmol VIP。对照组大鼠给予生理盐水。在注射后6 h、24 h处死大鼠,收集肺组织。采用逆转录聚合酶链反应(RT-PCR)检测肺组织中TLR2 mRNA和TLR4 mRNA的表达。在注射LPS 24 h后,通过光学显微镜和电子显微镜观察肺组织的病理变化。
结果
(1)肺组织病理学:LPS休克组肺泡腔内充满白细胞、坏死细胞、节段性出血和蛋白渗出。部分肺泡腔扩大,可见肺间质水肿。然而,LPS + VIP组的病理变化比LPS休克组轻。(2)与对照组相比,LPS休克组TLR2 mRNA和TLR4 mRNA的表达显著升高(F = 16.638,P = 0.000;t = 5.876,P = 0.000),LPS + VIP休克亚组24 h时TLR2 mRNA和TLR4 mRNA的表达低于LPS休克亚组(F = 16.676,P = 0.000;t = 3.946,P < 0.001)。
结论
LPS诱导的大鼠肺损伤中TLR2 mRNA和TLR4 mRNA的表达上调。VIP减轻了LPS诱导的肺损伤,这可能与TLR2 mRNA和TLR4 mRNA表达下调有关。VIP的作用可能提示了脓毒症中的一种保护机制。VIP可能在严重感染中发挥潜在的保护作用。
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