X连锁凋亡抑制蛋白反义寡核苷酸逆转K562细胞及难治性癫痫大鼠对卡马西平和苯妥英钠耐药性

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X连锁凋亡抑制蛋白反义寡核苷酸逆转K562细胞及难治性癫痫大鼠对卡马西平和苯妥英钠耐药性
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基金项目:上海市自然科学基金项目(09ZR1405500), 上海市卫生局局级科研项目(2008-80)和复旦大学生物医学研究院开放课题(2007)资助项目

Antisense Oligonucleotides of XIAP Reverse Resistance to Phenytoin and Carbamazepine in K562 Cells and Rats of Intractable Epilepsy

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This work was supported by grants from The Natural Science Foundation of Shanghai (09ZR1405500), The Research Projects of Shanghai Municipal Health Bureau (2008-08) and The Open Funds of Institutes of Biomedical Sciences Fudan University (2007)

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凋亡在癫痫发生机制中起重要作用，但其在难治性癫痫耐药机制中的作用尚不清楚．为研究X连锁凋亡抑制蛋白(X-linked inhibitor of apoptosis protein， XIAP)反义寡核苷酸对K562/Dox(阿霉素诱导)耐药细胞及难治性癫痫大鼠耐药性的影响，首先建立耐药的K562/Dox细胞株，比较XIAP在耐药细胞株和正常K562细胞株的表达情况，观察转染XIAP反义寡核苷酸后，线粒体膜电位变化以及对卡马西平和苯妥英钠耐药性的影响．另外，建立慢性杏仁核点燃癫痫模型，筛选出耐药组和药物敏感组，通过侧脑室注射XIAP反义寡核苷酸，对照组注射生理盐水．观察其对各组大鼠后放电阈值(after discharge threshold，ADT)、后放电时程(after discharge duration，ADD)等电生理指标的影响．结果发现，XIAP在K562/Dox耐药细胞上的表达明显高于正常K562细胞，XIAP反义寡核苷酸转染K562/Dox耐药细胞后，XIAP的表达明显下降．导致了K562/Dox细胞线粒体跨膜电位的下降，而且对苯妥英钠和卡马西平的耐药性明显下降，IC₅₀分别由(1 978.2 ± 90.3) mg/L和(1 875.6 ± 83.2) mg/L，降低到(1 123.5 ± 54.2) mg/L和(1 084.5 ± 60.6) mg/L，逆转倍数分别为1.76和1.73．同时动物实验发现，耐药组大鼠在给予XIAP反义寡核苷酸后，ADT明显高于对照组(P < 0.05)， ADD时程也明显缩短．上述结果证明，XIAP在耐药的K562/Dox细胞株存在高表达，下调XIAP在K562/Dox细胞株表达可以改善K562/Dox对卡马西平和苯妥英钠的耐药性．而且下调XIAP表达可以协助AEDs改善耐药大鼠的电生理活动，提示XIAP参与了难治性癫痫的耐药．

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There is accumulating evidence that apoptosis plays a key role in genesis of epilepsy, but the relationship between apoptosis and drug resistance in medically intractable epilepsy is not clear. The effect of XIAP antisense oligonucleotides on drug resistance in K562/Dox cells and rats of intractable epilepsy was investigated. The multidrug resistance cell line K562/Dox was established, and the expression of XIAP in K562/Dox cells and normal K562 cells was observed. After XIAP antisense oligonucleotides was transiently transfected into K562/Dox cells, mitochondrial membrane potential was assessed using JC-1. At the same time, antiepileptic drugs resistant in K562/Dox cells was measured by MTT. In addition, the model of intractable epilepsy was established by kindling of amygdale in rats. After XIAP antisense oligonucleotides was applied to PHT-CBZ resistant rats by lateral ventricle, after discharge threshold(ADT) and after discharge duration(ADD) was observed. The results showed that the expression of XIAP was significantly increased in K562/Dox cells compared with K562 cells. After XIAP antisense oligonucleotides was transiently transfected into K562/Dox cells, the expression of XIAP was regulated down, and mitochondrial membrane potential of K562/Dox cells was decreased. Moreover, XIAP down-regulation could increase the sensitivity of K562/Dox cells to antiepileptic drugs. The level of IC₅₀ was decreased significantly in K562/Dox cells, and the reversal index were 1.76 and 1.73, respectively. Furthermore, animal studies found that, compared with control group, ADT was significantly higher (P < 0.05) and ADD shortened in PHT-CBZ resistant rats after XIAP antisense oligonucleotides was applied. It is obvious that the expression of XIAP was significantly increased in drug resistant K562/Dox cells. Down-regulation of XIAP could reverse the drug-resistance of K562/Dox cells, and improve the electrobiological activity in PHT-CBZ resistant rats. These findings indicate that XIAP is involved in multidrug resistance in medically intractable epilepsy.

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陈英辉,王乃东,祖衡兵,洪震. X连锁凋亡抑制蛋白反义寡核苷酸逆转K562细胞及难治性癫痫大鼠对卡马西平和苯妥英钠耐药性[J].生物化学与生物物理进展,2010,37(6):635-640

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收稿日期:2009-11-30
最后修改日期:2010-01-21
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在线发布日期: 2010-01-26
出版日期: 2010-06-20

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