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西洛他唑和阿司匹林预处理对大鼠随后短暂性局灶性脑缺血的影响。

The effect of cilostazol and aspirin pre-treatment against subsequent transient focal cerebral ischemia in rat.

作者信息

Toda Yusuke, Katsura Ken-Ichiro, Saito Moeko, Inaba Toshiki, Sakurazawa Makoto, Katayama Yasuo

出版信息

Neurol Res. 2014 Nov;36(11):1011-9. doi: 10.1179/1743132814Y.0000000389. Epub 2014 May 18.

DOI:10.1179/1743132814Y.0000000389
PMID:24836463
Abstract

OBJECTIVES

Among several anti-platelet drugs to prevent recurrent stroke, cilostazol has shown various effects besides its anti-platelet activity. We examined whether 7 days of oral administration of cilostazol protects against subsequent cerebral ischemia, and whether or not the effect of combination therapy with aspirin is more protective.

METHODS

We used Sprague-Dawley (SD) rats and assigned them to four groups: vehicle, aspirin, cilostazol, and aspirin plus cilostazol combination therapy. After oral administration of anti-platelets for 7 days, we performed transient middle cerebral artery occlusion (MCAO) for 90 minutes, and examined infarct volume, neurological symptoms, and regional cerebral blood flow (rCBF). Immunostaining of Bax, Bcl-2, TUNEL, 4-HNE, 8-OHdG, and COX-2 was performed 24 hours after ischemia.

RESULTS

The cilostazol group and the combination therapy group showed significant decreases of infarct volume and significant improvements of rCBF during ischemia, compared with the vehicle or aspirin group. Significant decreases of Bax, TUNEL, 8-OHdG, and 4-HNE expression in the combination therapy group, compared with those in the vehicle or aspirin group, were shown in the boundary zone. COX-2 expression was unexpectedly increased in the combination therapy group.

DISCUSSION

Aspirin co-administration did not inhibit this effect. The addition of the oral administration of cilostazol either alone or with aspirin administration may be beneficial for subsequent cerebral ischemic damage in terms of reducing infarct volume, improving rCBF during ischemia, inhibiting the apoptotic pathway, and reducing oxidative stress.

摘要

目的

在几种预防复发性中风的抗血小板药物中,西洛他唑除了具有抗血小板活性外,还显示出多种作用。我们研究了口服西洛他唑7天是否能预防随后的脑缺血,以及阿司匹林联合治疗的效果是否更具保护作用。

方法

我们使用Sprague-Dawley(SD)大鼠,并将它们分为四组:溶剂对照组、阿司匹林组、西洛他唑组和阿司匹林加西洛他唑联合治疗组。口服抗血小板药物7天后,我们进行了90分钟的短暂大脑中动脉闭塞(MCAO),并检测梗死体积、神经症状和局部脑血流量(rCBF)。缺血24小时后进行Bax、Bcl-2、TUNEL、4-HNE、8-OHdG和COX-2的免疫染色。

结果

与溶剂对照组或阿司匹林组相比,西洛他唑组和联合治疗组在缺血期间梗死体积显著减小,rCBF显著改善。与溶剂对照组或阿司匹林组相比,联合治疗组在边界区Bax、TUNEL、8-OHdG和4-HNE表达显著降低。联合治疗组中COX-2表达意外增加。

讨论

联合使用阿司匹林并未抑制这种作用。单独或与阿司匹林联合口服西洛他唑在减少梗死体积、改善缺血期间的rCBF、抑制凋亡途径和减轻氧化应激方面,可能对随后的脑缺血损伤有益。

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