[全反式维甲酸对脑卒中小鼠脑缺血损伤及调节性T细胞计数的影响]
[Effect of all-trans retinoic acid on cerebral ischemia injury and regulatory T cell accounts in stroke mice].
作者信息
Yang Yanmei, Wang Shiquan, Jia Wenyuan, Dong Hailong, Wang Chen
机构信息
Department of Anesthesiology, Xijing Hospital, Fourth Military Medical University, Xi'an 710032, China.
出版信息
Xi Bao Yu Fen Zi Mian Yi Xue Za Zhi. 2014 May;30(5):458-61.
OBJECTIVE
To investigate the cerebral infarct volume 24 hours after transient middle cerebral artery occlusion (tMCAO) and the proportion of CD4⁺;CD25⁺;Foxp3⁺; regulatory T cells (Tregs) in splenocytes in diverse periods after all-trans retinoic acid (ATRA) treatment in mice, so as to explore whether ATRA have the protection against cerebral ischemia damage in mice through intervening Treg differentiation.
METHODS
Sixty male Kunming mice were randomly divided into two groups, i.e. pretreatment (n=40) and post-treatment (n=20) groups. Each group was against divided into two subgroups, i.e. tMCAO combined with ATRA treatment group, tMCAO combined with DMSO control group. Pretreatment groups: mice were treated intraperitoneally with ATRA (10 mg/kg) dissolved in 100 mL/L DMSO or equivalent volume of 100 mL/L DMSO daily for 7 days (n=20/group). Ten mice in each group were sacrificed and the proportion of Tregs in splenocytes was analyzed by flow cytometry (FCM) after 7-day pretreatment. The other 10 mice in each group were subjected to tMCAO by modified monofilament method. Neurologic deficit score (NDS) was recorded and the infarct volume was assessed by 2, 3, 5-triphenyltetrazolium chloride(TTC) staining 24 hours after tMCAO. The mice in post-treatment groups were treated intraperitoneally with ATRA (10 mg/kg) or equivalent volume of 100 mL/L DMSO immediately after the reperfusion of tMCAO modeling (n=10/group). NDS and infarct volume were assessed and the proportion of Tregs in splenocytes was analyzed 24 hours after tMCAO.
RESULTS
ATRA pretreatment for 7 days failed to improve neurologic function deficit (P>0.05) and to reduce the cerebral infarct volume (P>0.05) 24 hours after tMCAO in mice. ATRA post-treatment could markedly improve neurologic function (P<0.05) and reduce the cerebral infarct volume (P<0.05) 24 hours after tMCAO. However, neither ATRA pretreatment nor post-treatment had effect on the proportion of Tregs in the splenocytes of mice (P>0.05).
CONCLUSION
ATRA administered before tMCAO for 7 days failed to protect brain against ischemic damage. ATRA administered immediately following tMCAO induced cerebral protective effect 24 hours after tMCAO. The results suggest that Tregs change is not involved in the neuroprotection mechanism of ATRA.
目的
研究小鼠短暂性大脑中动脉闭塞(tMCAO)24小时后的脑梗死体积,以及全反式维甲酸(ATRA)治疗后不同时期脾细胞中CD4⁺;CD25⁺;Foxp3⁺调节性T细胞(Tregs)的比例,以探讨ATRA是否通过干预Treg分化对小鼠脑缺血损伤具有保护作用。
方法
将60只雄性昆明小鼠随机分为两组,即预处理组(n = 40)和治疗后组(n = 20)。每组再分为两个亚组,即tMCAO联合ATRA治疗组、tMCAO联合二甲基亚砜(DMSO)对照组。预处理组:小鼠每日腹腔注射溶于100 mL/L DMSO的ATRA(10 mg/kg)或等量体积的100 mL/L DMSO,共7天(每组n = 20)。每组10只小鼠在预处理7天后处死,通过流式细胞术(FCM)分析脾细胞中Tregs的比例。每组另外10只小鼠采用改良单丝法进行tMCAO。记录神经功能缺损评分(NDS),并在tMCAO后24小时通过2,3,5-氯化三苯基四氮唑(TTC)染色评估梗死体积。治疗后组小鼠在tMCAO模型再灌注后立即腹腔注射ATRA(10 mg/kg)或等量体积的100 mL/L DMSO(每组n = 10)。在tMCAO后24小时评估NDS和梗死体积,并分析脾细胞中Tregs的比例。
结果
ATRA预处理7天未能改善小鼠tMCAO后24小时的神经功能缺损(P>0.05),也未能减小脑梗死体积(P>0.05)。ATRA治疗后可显著改善tMCAO后24小时的神经功能(P<0.05),并减小脑梗死体积(P<0.05)。然而,ATRA预处理和治疗后均对小鼠脾细胞中Tregs的比例无影响(P>0.05)。
结论
tMCAO前7天给予ATRA未能保护脑免受缺血损伤。tMCAO后立即给予ATRA可在tMCAO后24小时诱导脑保护作用。结果表明,Tregs变化不参与ATRA的神经保护机制。
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