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降钙素和 α-CGRP 缺乏的老龄模型中,RANKL 相关抑制颗粒诱导的骨溶解。

RANKL-associated suppression of particle-induced osteolysis in an aged model of Calcitonin and α-CGRP deficiency.

机构信息

Department of Trauma Surgery, University of Duisburg-Essen, Essen, Germany.

出版信息

Biomaterials. 2013 Apr;34(12):2911-9. doi: 10.1016/j.biomaterials.2013.01.034. Epub 2013 Jan 26.

DOI:10.1016/j.biomaterials.2013.01.034
PMID:23357366
Abstract

An aging population with higher bone turnover intensifies the need for joint replacement surgery. However, particle-induced osteolysis (PIO) remains a major cause of early implant loosening. Differences in bone remodeling between young and aged Calcitonin (CT)- and α-CGRP (Calcitonin gene-related peptide)-deficient mice (Calca(-/-)) might modify our previous findings regarding CT/α-CGRP in PIO. This may have important implications for PIO in an aging population. Four groups of twelve-month-old wild-type and Calca(-/-) mice underwent either SHAM surgery with and without CT, or polyethylene-particle implantation with related treatment. Morphometric changes were detected using μ-CT, histomorphometric analysis and by counting TRAP(+) cells (osteoclast-staining). Bone remodeling was assessed using serum and urinary markers. There was no osteolysis in aged particle-treated Calca(-/-) animals and the effect of CT on PIO was reduced compared to wild-type mice. However, there were significantly higher numbers of TRAP(+) cells in Calca(-/-) animals, and bone remodeling markers revealed a significant increase in OPG/OCN and a significant reduction in RANKL compared to aged wild-type mice. CT/α-CGRP modulates bone cell activity in PIO in aged mice in a way that is distinct from young animals. This may have implications for the treatment of PIO in the periprosthetic surface of joint replacements in an aging population.

摘要

人口老龄化和更高的骨转换率加剧了关节置换手术的需求。然而,颗粒诱导性骨溶解(PIO)仍然是导致早期植入物松动的主要原因。年轻和老年降钙素(CT)和α-CGRP(降钙素基因相关肽)缺陷小鼠(Calca(-/-))之间的骨重塑差异可能会改变我们之前关于 PIO 中 CT/α-CGRP 的发现。这可能对老龄化人口中的 PIO 具有重要意义。四组 12 个月大的野生型和 Calca(-/-)小鼠接受了假手术和 CT 治疗,或聚乙烯颗粒植入和相关治疗。使用μ-CT、组织形态计量学分析和 TRAP(+)细胞计数(破骨细胞染色)检测形态变化。使用血清和尿液标志物评估骨重塑。在老年颗粒处理的 Calca(-/-)动物中没有骨溶解,并且 CT 对 PIO 的影响比野生型小鼠降低。然而,Calca(-/-)动物中的 TRAP(+)细胞数量明显更高,骨重塑标志物显示 OPG/OCN 显著增加,RANKL 显著降低,与老年野生型小鼠相比。CT/α-CGRP 以不同于年轻动物的方式调节老年小鼠 PIO 中的骨细胞活性。这可能对治疗老龄化人口关节置换假体表面的 PIO 具有重要意义。

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