XIAP过度表达对顺铂耳毒性的拮抗作用（毕业设计-耳鼻咽喉科学专业）

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1、上海交通大学硕士学位论文XIAP 过度表达对顺铂耳毒性的拮抗作用姓名：和守睆申请学位级别：硕士专业：耳鼻咽喉科学指导教师：陈斌20090501第一部分小鼠顺铂耳毒性两种建模方法的比较摘要目的探索建立小鼠顺铂耳毒性模型安全有效的方法材料和方法选择月龄小鼠只将其分成四组每组只局部给药两组通过左侧后半规管分别注射生理盐水后半规管

2、生理盐水组及顺铂后半规管顺铂组这两组小鼠破坏右侧耳蜗后检测随即左耳给药给药后第七天再行检测然后处死动物行耳蜗基底膜毛细胞计数全身给药两组腹腔注射的利尿酸后其中一组肌肉注射的顺铂另一组肌肉注射的顺铂这两组小鼠于给药后第七天处死行耳蜗基底膜毛细胞计数结果后半规管生理盐水组给药前后阈移无统计学意义后半规管顺铂组给

3、药前后阈移有统计学意义后半规管顺铂组给药前后阈移与后半规管生理盐水组相比有统计学差异后半规管顺铂组毛细胞缺失数与后半规管生理盐水组相比有统计学差异全身给药的两组动物毛细胞缺失数相比也有统计学差异局部给药组给药后一周内全身情况良好无死亡全身给药组给药后一周内全身情况欠佳每组各有只死亡结论后半规管给药是建立

4、小鼠顺铂耳毒性模型安全有效的途径全身联合应用顺铂和利尿酸极易造成小鼠死亡不宜用来建立小鼠顺铂耳毒性模型关键词顺铂耳毒性小鼠第二部分过度表达对顺铂耳毒性的拮抗作用摘要目的探讨连锁凋亡抑制蛋白过度表达能否在小鼠体内拮抗顺铂耳毒性材料和方法选择同源月龄小鼠只利用技术分成野生小鼠及转基因小鼠将其分成六组小鼠只通过左侧后半规管注射生理盐水生理盐水组小鼠顺铂组及小鼠顺铂组各

5、只通过左侧后半规管注射顺铂这三组小鼠破坏右侧耳蜗后检测随即左耳给药给药后第七天再行检测然后处死动物行耳蜗基底膜毛细胞计数小鼠只通过双侧后半规管注射生理盐水小鼠及小鼠各只通过双侧后半规管注射顺铂这三组小鼠于给药后第七天处死行螺旋神经节细胞计数及血管纹横截面积测算结果生理盐水组给药前后阈移无统计学意义顺铂组及顺铂组给药前后阈移均有统计学意义三组动物给药前

6、后阈移两两相比均有统计学差异三组动物毛细胞缺失数及螺旋神经节细胞计数两两相比均有统计学差异血管纹横截面积两两相比均无统计学差异结论顺铂可以造成小鼠听力损失毛细胞及螺旋神经节细胞缺失对血管纹横截面积无明显影响过度表达可以在一定程度上拮抗顺铂所致的听力损失毛细胞及螺旋神经节细胞缺失对血管纹横截面积无明显影响

7、关键词顺铂耳毒性小鼠 PART ONEA COMPARISON OF TWO APPROACHES TOESTABLISH MODELS OF CISPLATININDUCED COCHLEAR LESION IN C57 MICEABSTRACTObjective: To explore a safe and effective approach to establish cisplatininduced cochlear lesion in C57BL/6J mice.Materials and methods: 24 C57BL/6J adult mice (aged 2

8、 months) enrolledin this study were assigned to four groups, 6 mice in each group. The localadministration groups included two groups, which received NS (normal saline,NS) and cisplatin respectively through the left posterior semicircular canalinjection. The right ears of the two groups were destroy

9、ed and ABR (auditorybrainstem response, ABR) was recorded, and the drugs were injected into theleft ears immediately after ABR recording; ABR was recorded 1 week afterthe injection, and then the cochleae were collected for establishingcytocochleogram. The systemic administration groups included two

10、groups,which were both given EA (ethacrynic acid, EA, 40 mg/kg, i.p.); then onegroup was given cisplatin (0.3 mg/kg, i.m.), and the other group was givencisplatin (0.5 mg/kg, i.m.). The cochleae of the two groups were collected forestablishing cytocochleogram 1 week after the injection.Results: NS i

11、njection through the posterior semicircular canal didnt displayany ABR threshold shift after the injection, while cisplatin injection through theposterior semicircular canal showed profound ABR threshold shifts after theinjection; there was significant difference in ABR threshold shifts between NSin

12、jection and cisplatin injection through the posterior semicircular canal afterthe injection. There was significant difference in HC (hair cell, HC) lossbetween NS injection and cisplatin injection through the posterior semicircularcanal, and significant difference in HC loss was found between the tw

13、ogroups receiving cisplatin and EA systematically. The animals of the localadministration groups were in good condition and there was no death duringthe week after the injection, however, the animals of the systemicadministration groups were in poor condition and 4 mice of each group diedduring the

14、week after the injection.Conclusions: The posterior semicircular canal injection is a safe and effectiveapproach to establish cisplatin induced cochlear lesion in mice; the systemicadministration of cisplatin and EA can easily induce mice to death, so itsunsuitable to establish cisplatin induced cochlear lesion in mice.KEY WORDS: cisplatin, ototoxicity, C57 micePART TWOOVER EXPRESSION OF XIAP PROTECTSAGAINST CISPLATIN OTOTOXICITYABSTRACTObjective: To explore whether over expression of XIAP (X-linked inhibitorof apoptosis protein, XIAP) can protect against cisplatin otot

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