TLR4干扰RNA腺病毒的构建及其对肺泡巨噬细胞内毒素反应的影响  被引量:2

Construction of the adenovirus expressing rats expressing TLR4 siRNA and its effect on alveolar macrophage reaction to LPS

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作  者:吴飞翔[1] 吕欣[1] 俞卫锋[1] 黄盛东 徐学武[1] 孙玉明[1] 袁扬 卞金俊[3] 

机构地区:[1]解放军第二军医大学东方肝胆外科医院麻醉科,上海200438 [2]解放军胸心外科研究所,上海200433 [3]解放军第二军医大学长海医院麻醉科,上海200433

出  处:《中国急救医学》2008年第3期230-234,289,共6页Chinese Journal of Critical Care Medicine

基  金:国家自然基金资助项目(No30700788)

摘  要:目的构建表达大鼠TLR4siRNA的腺病毒,并观察对内毒素诱导的大鼠肺泡巨噬细胞TLR4的抑制和TNF-α、IL-10释放的影响。方法合成双链寡核苷酸并克隆入pShuttleH1载体,pShuttleH1-TLR4线性化后电转化到含pAdEasy-1的BJ5183感受态细菌中获取重组质粒,重组质粒用脂质体转染293细胞获取重组腺病毒Ad-siTLR4;扩增、纯化腺病毒,TCID50法测定病毒滴度。原代培养大鼠肺泡巨噬细胞,腺病毒Ad-siTLR4感染后加入内毒素,采用RT-PCR和Western blot观察TLR4蛋白及mRNA的表达,ELISA检测TNF-α、IL-10的释放情况。结果目的基因序列正确并成功克隆入腺病毒,腺病毒Ad-siTLR4滴度为5.72×109pfu/mL。转染腺病毒后的内毒素诱导的肺泡巨噬细胞TLR4蛋白和mRNA水平下降,TNF-α、IL-10的表达均明显减弱。结论本研究成功构建了表达大鼠TLR4 siRNA的腺病毒,具有良好的抑制TLR4和TNF-α、IL-10的作用,为下一步动物体内实验基因治疗急性肺损伤奠定良好的基础。Objective To construct the incompetent -replication adenovirus expressing rats TLR4 siRNA and to identify its effect on alveolar macrophage reaction to LPS ( Lipopolysaccharide ) in vitro. Methods The complementary DNA containing both sense and antisense Oligo DNA of the targeting sequence was cloned into the pShuttleH1 vector. Linearized pShuttleH1 - siTLR4 was transformed into E. coli BJ5183 cells containing backbone plasmid pAdEasy- 1 by electroporation. The recombinant plasmid was transfected into 293 cells to package the adenovirus Ad - siTLR4. The titers of adenovirus were determined using the specific 50% tissue culture infection dosage (TCID50) method. After virus infected the cultured alveolar macrophage, the effect on LPS - induced TLR4 protein and its mRNA expression were observed by western blot and RT- PCR. TNF -α, IL- 10 expression were also detected by ELISA. Resuits It was identified that the sequence of gene was correctly inserted into the genome of virus. The titer of recombinant adenovirus was 5.72 × 10^9pfu/mL. TLR4 protein and its mRNA expression were greatly reduced after virus infection. TNF - α, IL - 10 expression were also decreased. Conclusion The recombinant adenovirus expressing rats TLR4 siRNA were successfully constructed,which probably can be further used in treatment of acute lung injury in vivo.

关 键 词:TOLL样受体4 RNA干扰 腺病毒 TNF-α IL-10 

分 类 号:R346[医药卫生—基础医学]

 

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