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双膦酸盐对颗粒生物材料相关巨噬细胞诱导的骨吸收的抑制作用。

Bisphosphonate inhibition of bone resorption induced by particulate biomaterial-associated macrophages.

作者信息

Pandey R, Quinn J M, Sabokbar A, Athanasou N A

机构信息

Nuffield Department of Orthopaedic Surgery, University of Oxford, Headington, UK.

出版信息

Acta Orthop Scand. 1996 Jun;67(3):221-8. doi: 10.3109/17453679608994677.

DOI:10.3109/17453679608994677
PMID:8686457
Abstract

Aseptic loosening of total joint replacements is associated with bone resorption. A heavy infiltrate of foreign body macrophages in response to biomaterial wear particles is commonly found in the fibrous membrane surrounding loose components. It has recently been shown that foreign body macrophages can differentiate into osteoclastic cells. To determine whether pharmacological inhibitors of bone resorption have a role to play in controlling the osteolysis of aseptic loosening, we analyzed the effect of a bisphosphonate, disodium ethane-1, 1-diphosphonate (EHDP) on this process. Murine monocytes and foreign body macrophages (derived from granulomas formed by subcutaneous implantation of particles of prosthetic biomaterials) were co-cultured with UMR106 osteoblast-like cells in the presence of 1,25 dihydroxyvitamin D3 for 14 days on glass coverslips and bone slices. EHDP significantly inhibited bone resorption in these co-cultures. There was little or no expression of the osteoclast-associated enzyme, tartrate-resistant acid phosphatase (TRAP) in EHDP-treated co-cultures. Addition of EHDP to monocyte-UMR106 co-cultures after the appearance of TRAP-positive cells did not abolish bone resorption, indicating that EHDP, in addition to its known inhibitory effect on osteoclast function, suppresses differentiation of osteoclast precursors. EHDP inhibition of the osteolysis induced by particulate biomaterial-associated macrophages shows that pharmacological inhibition of bone resorption might be used to control the osteolysis of aseptic loosening.

摘要

全关节置换的无菌性松动与骨吸收有关。在松动部件周围的纤维膜中,常见大量异物巨噬细胞因生物材料磨损颗粒而浸润。最近研究表明,异物巨噬细胞可分化为破骨细胞。为确定骨吸收的药理抑制剂在控制无菌性松动的骨溶解中是否起作用,我们分析了一种双膦酸盐——乙烷-1,1-二膦酸二钠(EHDP)对该过程的影响。将小鼠单核细胞和异物巨噬细胞(源自皮下植入假体生物材料颗粒形成的肉芽肿)与UMR106成骨细胞样细胞在1,25-二羟基维生素D3存在下于玻璃盖玻片和骨切片上共培养14天。EHDP显著抑制了这些共培养体系中的骨吸收。在EHDP处理的共培养体系中,破骨细胞相关酶——抗酒石酸酸性磷酸酶(TRAP)几乎没有表达。在TRAP阳性细胞出现后向单核细胞-UMR106共培养体系中添加EHDP并不能消除骨吸收,这表明EHDP除了对破骨细胞功能有已知的抑制作用外,还抑制破骨细胞前体的分化。EHDP对颗粒生物材料相关巨噬细胞诱导的骨溶解的抑制作用表明,骨吸收的药理抑制可能用于控制无菌性松动的骨溶解。

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