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白介素-1受体拮抗蛋白的应用对早期创伤性关节炎软骨细胞代谢的影响

发布时间:2018-09-12 11:24
【摘要】:目的探讨应用白介素-1受体拮抗蛋白(IL1RA)对早期创伤性关节炎软骨细胞代谢的影响,主要观察应用后相关细胞炎性因子及蛋白酶基因的表达变化。方法 44只健康成年新西兰大白兔,随机分为对照(假手术)组(CON组,n=4)、安慰剂组(PBS组,n=20)、IL1RA治疗组(IL1RA组,n=20)。其中PBS组及IL1RA组均接受关节内重物击打,造成创伤性关节炎模型。造模后1 h,CON组不接受任何治疗,PBS组及IL1RA组实验兔膝关节则分别给予0.5 m L无菌PBS和0.5 m L IL1RA-PBS关节腔注射。术后3 h及8 h采集关节液,检测IL-1β含量。术后8 h处死动物取软骨组织进行软骨细胞培养后,测定细胞活力及凋亡率,RT-PCR检测软骨组织中ADAMTs-4、ADAMTs-5、MMP-3、IL-1β及TNF-α的m RNA表达。结果术后3 h及8 h,PBS组关节液中IL-1β的含量均明显高于CON组(P0.01)。然而,经IL1RA介入治疗后,IL-1β在术后各测试点的含量均明显低于PBS组(P0.05)。与CON组相比,术后8h培养的PBS组软骨细胞活力明显降低(P0.05),而IL1RA组软骨细胞活力与CON组相比无显著性差异,但明显高于PBS组。另一方面,与CON组及IL1RA组相比,PBS组的细胞凋亡率明显增高(P0.05)。而IL1RA组与CON组相比,细胞凋亡率无明显差别(P0.05)。RT-RCR结果显示,与CON组比较,PBS组所有目的基因m RNA的表达均明显增加(P0.01)。然而,IL1RA组所有目的基因的表达与CON组相比无统计学差异,但明显低于PBS组(P0.01)。结论实验结果表明创伤后关节炎早期应用IL1RA介入治疗可有效降低关节液细胞炎性因子的浓度,抑制细胞炎性因子对软骨细胞生长增殖的负性影响,降低细胞凋亡,且对于促进软骨细胞基质降解的细胞炎性因子及蛋白酶的表达显著下调,对PTOA病程发展具有抑制作用。
[Abstract]:Objective to investigate the effect of interleukin-1 receptor antagonist protein (IL1RA) on the metabolism of chondrocytes in early traumatic arthritis. Methods 44 healthy adult New Zealand white rabbits were randomly divided into control (sham operation) group (CON group), placebo group (PBS group, n = 20) and IL1RA treatment group (IL1RA group, n = 20). PBS group and IL1RA group were all hit by intra-articular heavy objects to make traumatic arthritis model. One hour after modeling, the rabbits in the Con group were injected with 0.5 mL aseptic PBS and 0.5 mL IL1RA-PBS respectively in the knee joint without any treatment. Articular fluid was collected at 3 h and 8 h after operation to detect the content of IL-1 尾. Chondrocytes were harvested from chondrocytes 8 hours after operation, and the cell viability and apoptosis rate were measured. The m RNA expression of ADAMTs-4,ADAMTs-5,MMP-3,IL-1 尾 and TNF- 伪 in chondrocytes was detected by reverse transcription-polymerase chain reaction (RT-PCR). Results the content of IL-1 尾 in articular fluid of PBS group was significantly higher than that of CON group at 3 h and 8 h postoperatively (P0.01). However, the level of IL-1 尾 in all test points after IL1RA intervention was significantly lower than that in PBS group (P0.05). Compared with CON group, the chondrocyte activity of PBS group was significantly lower than that of CON group (P0.05), but the chondrocyte activity of IL1RA group was not significantly different from that of CON group, but significantly higher than that of PBS group. On the other hand, compared with CON group and IL1RA group, the apoptosis rate of PBS group was significantly higher (P0.05). There was no significant difference in apoptosis rate between IL1RA group and CON group (P0.05). RT-RCR results showed that the expression of m RNA in CON group was significantly higher than that in CON group (P0.01). However, the expression of all target genes in the IL1RA group was not significantly different from that in the CON group, but was significantly lower than that in the PBS group (P0.01). Conclusion the experimental results show that early IL1RA intervention therapy can effectively reduce the concentration of inflammatory cytokines in articular fluid, inhibit the negative effects of cytokines on the growth and proliferation of chondrocytes, and reduce apoptosis. The expression of inflammatory cytokines and protease, which can promote the degradation of chondrocyte matrix, was significantly down-regulated and inhibited the progression of PTOA.
【作者单位】: 西安工业大学高水平运动管理中心;昆明学院体育学院;渭南市第一医院重症医学科;
【分类号】:R873

【参考文献】

相关期刊论文 前4条

1 罗韬;刘炀;范伟杰;;关节软骨损伤基因治疗研究进展[J];中国矫形外科杂志;2016年08期

2 邵俊杰;张先龙;蒋W,

本文编号:2238860


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