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作 者:张紫机[1] 康焱[1] 杨子波[1] 侯昌禾[1] 黄广鑫[1] 陈蔚深 盛璞义[1] 何爱珊[1] 傅明[1] 廖威明[1] 张志奇[1]
机构地区:[1]中山大学附属第一医院关节外科,广东省广州市510080
出 处:《中国组织工程研究》2015年第15期2297-2304,共8页Chinese Journal of Tissue Engineering Research
基 金:国家自然科学基金资助项目(81171709;81301558;81371941;81201388);教育部高等学校博士点基金新教师类资助项目(20130171120074);广东省自然科学基金博士启动项目(S2013040016269)~~
摘 要:背景:既往研究表明抵抗素可刺激软骨细胞产生大量趋化因子,在炎症性关节病变中具重要作用,但具体作用机制未明。目的:进一步探讨抵抗素刺激软骨细胞趋化因子CCL3及CCL4基因表达上调的机制。方法:培养人源性软骨细胞,T/C-28a2细胞及ATDC5细胞,采用q PCR检测抵抗素刺激趋化因子基因的作用,C/EBPβ表达,核因子κB亚型及软骨特异性mi RNAs。给予核因子κB抑制剂(IKK-NBD)和C/EBPβ抑制剂(SB303580),对C/EBPβ及核因子κB的共同调节作用进行检测。在给予抵抗素刺激或无抵抗素刺激时分别进行亚细胞结构定位检测。结果与结论:1抵抗素可非依赖性上调趋化因子基因表达。2软骨细胞对抵抗素刺激应答具有非严格细胞特异性,通过C/EBPβ抑制剂、核因子κB及一些软骨细胞特异性mi RNAs,可对趋化因子基因表达进行联合调控。3一过性核因子κB活性增高可增强C/EBPβ活性,且两个转录因子对趋化因子基因CCL3及CCL4的作用均为非依赖性。BACKGROUND: Previous studies have indicated that resistin stimulates a large set of chemokines in chondrocytes that are known to be important in inflammatory joint lesions. OBJECTIVE: To further investigate the mechanism of co-regulation roles of transcription and post-transcription in the up-regulation of two chemokine genes CCL3 and CCL4 in chondrocytes in response to resistin. METHODS: Human chondrocytes, T/C-28a2 and ATDC5 cells were cultured. The function of resistin on the chemokine genes, and the expression of C/EBPβ, nuclear factor-κB isoforms and chondrogenic specific mi RNAs were tested by q PCR. The co-regulation of C/EBPβ and nuclear factor-κB was investigated by nuclear factor-κB inhibitor(IKK-NBD) and C/EBPβ inhibitor(SB303580) treatments, and subcellular localization was detected with or without resistin stimulation. RESULTS AND CONCLUSION: Resistin could increase the expression of chemokine genes independently. Chondrocytes reacted in a non-restrictedly cell-specific manner to resistin; C/EBPβ inhibitor, nuclear factor-κB and some chondrogenic specific mi RNAs in a combinatorial manner regulated chemokine gene expression. Theactivity of C/EBPβ was augmented by a transient increase in activity of nuclear factor-κB, and both transcription factors acted independently on the chemokine genes, CCL3 and CCL4.
关 键 词:软骨细胞 趋化因子类 NF-κB 组织构建 软骨组织工程 抵抗素 趋化因子 CCL3 CCL4 转录调控 C/EBPΒ 核因子κB 转录后调控 miRNAs 国家自然科学基金
分 类 号:R318[医药卫生—生物医学工程]
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