布洛芬对大鼠皮质缺血半暗带酸敏感离子通道的作用

李栋; 彭鹏; 张永一; 袁维秀; 刘晓燕

doi:10.3969/j.issn.2095-5227.2017.08.016

布洛芬对大鼠皮质缺血半暗带酸敏感离子通道的作用

Role of ibuprofen in protecting cerebral ischemia-reperfusion injury by affecting cortical ischemic penumbra acid-sensitive ion channel proteins

摘要

摘要: 目的研究布洛芬对大鼠皮质缺血半暗带酸敏感离子通道的影响，探讨其对脑缺血再灌注损伤的保护作用及机制。方法健康雄性成年SD大鼠随机分为4组：假手术+溶媒(S+R)组、假手术+布洛芬(S+B)组、模型+溶媒(C+R)组、模型+布洛芬(C+B)组，每组12只。假手术组只分离血管，不进行栓塞；模型组常规建立大脑中动脉阻塞(middle cerebral artery occlusion，MCAO)模型；布洛芬组于大脑中动脉阻塞前1 h及之后每隔8 h腹腔注射布洛芬(80 mg/kg)，共240 mg/(kg· 24 h)；溶媒组于相同时间点腹腔注射相应体质量的精氨酸溶液。术后24 h进行神经行为学评分、TTC染色观察脑梗死容积和Western blot检测皮质缺血半暗带酸敏感离子通道1a(acid-sensing ion channel 1a，ASIC1a)和酸敏感离子通道2a(acidsensing ion channel 2a，ASIC2a)的总蛋白表达和膜蛋白含量。结果大鼠神经行为学评分C+R组(6.06±0.35)与S+R组(17.56±0.15)大鼠相比明显降低(P＜ 0.05)；C+B组神经行为学评分(11.94±0.33)与C+R组相比有所提高(P＜ 0.05)，且脑梗死容积百分比前者(11.24%±0.93%)较后者(20.03%±1.74%)明显减小(P＜ 0.01)；C+R组大鼠皮质缺血半暗带ASIC1a总蛋白的相对表达水平(0.99±0.07)与S+R组(1.00±0.04)相比没有明显差异(P=0.12)，但ASIC1a膜蛋白的含量明显升高(1.40±0.11 vs 0.96±0.04，P＜ 0.05)、ASIC2a总蛋白的表达明显增加(1.87±0.14 vs 0.98±0.07，P＜ 0.01)，C+B组ASIC1a的总蛋白表达水平(0.79±0.08)与C+R组(0.99±0.07)相比有所下调，但差异无统计学意义(P=0.07)，C+R组较C+B组ASIC1a膜蛋白的含量(1.40±0.11 vs 0.98±0.12)以及ASIC2a总蛋白的表达(1.87±0.14 vs 1.18±0.12)明显增加(P＜ 0.05)。结论布洛芬能明显改善大鼠MCAO术后的神经行为学障碍、缩小脑梗死容积，这种作用可能通过抑制ASIC2a的表达上调，减少ASIC1a的膜蛋白含量。

Abstract: Objective To study the effect of ibuprofen on acid-sensitive ion channels in rat's cortical ischemic penumbra and investigate its protective effect on cerebral ischemia-reperfusion injury and its mechanism. Methods Forty-eight healthy male adult SD rats were randomly divided into 4 groups: sham operation + vehicle group (S + R), sham operation + ibuprofen group (S + B), model + vehicle group (C + R), model + ibuprofen group (C + B) with 12 in each group. Sham operation group only received separating blood vessels without embolization. Middle cerebral artery occlusion (MCAO) was used to establish the modal. Ibuprofen (240 mg/kg·day) was delivered with 80 mg/kg intraperitoneally at 1 h before MCAO and every 8 hours thereafter, for a total of three injections in the ibuprofen group. Rats in the vehicle group were injected intraperitoneally with equivolumetric arginine vehicle. The neuroprotective effect of ibuprofen was evaluated at 24 h after MCAO by neurobehavioral score and TTC staining. The effect of ibuprofen on the expressions of ASIC1a and ASIC2a protein in cortical ischemic penumbra was assessed by western blot. Results Compared with S + R group (17.56±0.15), the neurological score of C + R group (6.06±0.35) decreased significantly (P＜ 0.05). Compared with C + R group, the neurological score of C + B group (11.94±0.33) increased (P＜ 0.05), and the percentage of cerebral infarction volume decreased significantly (C+B 11.24%±0.93% vs C+R 20.03%±1.74%, P＜ 0.01). There was no significantdifference in the relative expression level of ASIC1a (0.99±0.07) in the cortical ischemic penumbra of C + R group compared with S + R group (1.00±0.04) (P=0.12), while the content of ASIC1a membrane protein (1.40±0.11 vs 0.96±0.04, P＜ 0.05) and the expression level of ASIC2a (1.87±0.14 vs 0.98±0.07, P＜ 0.01) significantly increased. Compared with C + R group, the expression level of ASIC1a was down-regulated, but the difference was not statistically significant (0.79±0.08 vs 0.99±0.07, P=0.07). The content of ASIC1a membrane protein (1.40±0.11 vs 0.98±0.12) and the expression of ASIC2a in C+B group (1.87±0.14 vs 1.18±0.12) were significantly lower than those in C + R group (P＜ 0.05, respectively). Conclusion Ibuprofen has neuroprotective effect, which may be achieved by inhibiting the up-regulation of ASIC2a and reducing the protein content of ASIC1a.

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