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白细胞介素-1受体拮抗剂(IL-1Ra)或病毒白细胞介素-10(vIL-10)基因转移对磨损颗粒诱导的小鼠骨溶解模型的保护作用。

Protective effects of IL-1Ra or vIL-10 gene transfer on a murine model of wear debris-induced osteolysis.

作者信息

Yang S-Y, Wu B, Mayton L, Mukherjee P, Robbins P D, Evans C H, Wooley P H

机构信息

Department of Orthopaedic Surgery, Wayne State University, Detroit, MI, USA.

出版信息

Gene Ther. 2004 Mar;11(5):483-91. doi: 10.1038/sj.gt.3302192.

Abstract

The current study evaluated the protective effects of anti-inflammatory cytokine gene transfer on osteolysis provoked by orthopedic biomaterial particles using a murine model of inflammatory bone loss. A section of bone was surgically implanted into an air pouch established on a syngeneic recipient mouse. Inflammation was provoked by introduction of ultra-high-molecular-weight polyethylene (UHMWPE) particles into the pouch, and retroviruses encoding for interleukin-1 receptor antagonist (hIL-1Ra), viral interleukin-10 (vIL-10), or LacZ genes were injected. Pouch fluid and tissue were harvested 7 days later for histological and molecular analyses. The results indicated that IL-1Ra or vIL-10 gene transfer significantly inhibited IL-1beta and tumor necrosis factor (TNF) expression at both mRNA and protein levels. There were significantly lower mRNA expressions of calcitonin receptor and cathepsin K in RNA isolated from hIL-1Ra- or vIL-10-transduced pouches than LacZ-transduced and virus-free controls. Both anti-inflammatory cytokine gene transfers significantly reduced the mRNA expression of M-CSF (70-90%) and RANK (>65%) in comparison with LacZ- and virus-free controls. Histological examination showed that hIL-1Ra or vIL-10 gene transfer dramatically abolished UHMWPE-induced inflammatory cellular infiltration and bone pit erosion compared to LacZ-transduced and virus-free controls. Histochemical staining revealed significantly fewer osteoclast-like cells in samples treated with IL-1Ra or vIL-10 gene transfer. In addition, bone collagen content was markedly preserved in the groups with anti-inflammatory cytokine gene transfers compared with the other two groups. Overall, retrovirus-mediated hIL-1Ra or vIL-10 gene transfer effectively protected against UHMWPE-particle-induced bone resorption, probably due to the inhibition of IL-1/TNF-induced M-CSF production and the consequent osteoclast recruitment and maturation.

摘要

本研究使用炎症性骨质流失的小鼠模型,评估了抗炎细胞因子基因转移对骨科生物材料颗粒引发的骨溶解的保护作用。将一段骨手术植入同基因受体小鼠建立的气袋中。通过向气袋中引入超高分子量聚乙烯(UHMWPE)颗粒引发炎症,并注射编码白细胞介素-1受体拮抗剂(hIL-1Ra)、病毒白细胞介素-10(vIL-10)或LacZ基因的逆转录病毒。7天后收集气袋液和组织进行组织学和分子分析。结果表明,IL-1Ra或vIL-10基因转移在mRNA和蛋白质水平上均显著抑制IL-1β和肿瘤坏死因子(TNF)的表达。从hIL-1Ra或vIL-10转导的气袋中分离的RNA中,降钙素受体和组织蛋白酶K的mRNA表达明显低于LacZ转导和无病毒对照。与LacZ和无病毒对照相比,两种抗炎细胞因子基因转移均显著降低了M-CSF(70-90%)和RANK(>65%)的mRNA表达。组织学检查显示,与LacZ转导和无病毒对照相比,hIL-1Ra或vIL-10基因转移显著消除了UHMWPE诱导的炎症细胞浸润和骨坑侵蚀。组织化学染色显示,IL-1Ra或vIL-10基因转移处理的样本中破骨细胞样细胞明显减少。此外,与其他两组相比,抗炎细胞因子基因转移组的骨胶原含量明显保留。总体而言,逆转录病毒介导的hIL-1Ra或vIL-10基因转移有效地防止了UHMWPE颗粒诱导的骨吸收,这可能是由于抑制了IL-1/TNF诱导的M-CSF产生以及随后的破骨细胞募集和成熟。

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