Bagi Cedo M, Berryman Edwin, Zakur David E, Wilkie Dean, Andresen Catharine J
Global Science and Technology, Pfizer Global Research and Development, Pfizer Inc., 100 Eastern Point Road, Groton, CT, 06340, USA.
Comparative Medicine, Global Science and Technology, Pfizer Global Research and Development, Pfizer Inc., 100 Eastern Point Road, Groton, CT, 06340, USA.
Arthritis Res Ther. 2015 Nov 6;17:315. doi: 10.1186/s13075-015-0829-5.
Osteoarthritis (OA) is a leading cause of disability, but despite the high unmet clinical need and extensive research seeking dependable therapeutic interventions, no proven disease-modifying treatment for OA is currently available. Due to the close interaction and interplay between the articular cartilage and the subchondral bone plate, it has been hypothesized that antiresorptive drugs can also reduce cartilage degradation, inhibit excessive turnover of the subchondral bone plate, prevent osteophyte formation, and/or that bone anabolic drugs might also stimulate cartilage synthesis by chondrocytes and preserve cartilage integrity. The benefit of intensive zoledronate (Zol) and parathyroid hormone (PTH) therapy for bone and cartilage metabolism was evaluated in a rat model of OA.
Medial meniscectomy (MM) was used to induce OA in male Lewis rats. Therapy with Zol and human PTH was initiated immediately after surgery. A dynamic weight-bearing (DWB) system was deployed to evaluate the weight-bearing capacity of the front and hind legs. At the end of the 10-week study, the rats were euthanized and the cartilage pathology was evaluated by contrast (Hexabrix)-enhanced μCT imaging and traditional histology. Bone tissue was evaluated at the tibial metaphysis and epiphysis, including the subchondral bone. Histological techniques and dynamic histomorphometry were used to evaluate cartilage morphology and bone mineralization.
The results of this study highlight the complex changes in bone metabolism in different bone compartments influenced by local factors, including inflammation, pain and mechanical loads. Surgery caused severe and extensive deterioration of the articular cartilage at the medial tibial plateau, as evidenced by contrast-enhanced μCT and histology. The study results showed the negative impact of MM surgery on the weight-bearing capacity of the operated limb, which was not corrected by treatment. Although both Zol and PTH improved subchondral bone mass and Zol reduced serum CTX-II level, both treatments failed to prevent or correct cartilage deterioration, osteophyte formation and mechanical incapacity.
The various methods utilized in this study showed that aggressive treatment with Zol and PTH did not have the capacity to prevent or correct the deterioration of the hyaline cartilage, thickening of the subchondral bone plate, osteophyte formation or the mechanical incapacity of the osteoarthritic knee.
骨关节炎(OA)是导致残疾的主要原因,但尽管临床需求未得到充分满足且开展了广泛研究以寻求可靠的治疗干预措施,但目前尚无经证实的可改变OA病情的治疗方法。由于关节软骨与软骨下骨板之间存在密切的相互作用,因此有人推测抗吸收药物也可减少软骨降解、抑制软骨下骨板的过度更新、预防骨赘形成,和/或骨合成代谢药物可能还会刺激软骨细胞合成软骨并维持软骨完整性。本研究在OA大鼠模型中评估了大剂量唑来膦酸(Zol)和甲状旁腺激素(PTH)治疗对骨和软骨代谢的益处。
采用内侧半月板切除术(MM)诱导雄性Lewis大鼠发生OA。术后立即开始使用Zol和人PTH进行治疗。采用动态负重(DWB)系统评估前肢和后肢的负重能力。在为期10周的研究结束时,对大鼠实施安乐死,并通过造影剂(Hexabrix)增强的μCT成像和传统组织学方法评估软骨病理学。在胫骨干骺端和骨骺,包括软骨下骨,对骨组织进行评估。采用组织学技术和动态组织形态计量学方法评估软骨形态和骨矿化情况。
本研究结果突出了受局部因素(包括炎症、疼痛和机械负荷)影响的不同骨腔室中骨代谢的复杂变化。造影剂增强的μCT和组织学结果表明,手术导致内侧胫骨平台的关节软骨严重且广泛地退化。研究结果显示,MM手术对手术肢体的负重能力有负面影响,且治疗未能纠正这一影响。尽管Zol和PTH均改善了软骨下骨量,且Zol降低了血清CTX-II水平,但两种治疗均未能预防或纠正软骨退化、骨赘形成和机械功能障碍。
本研究采用的各种方法表明,使用Zol和PTH进行积极治疗无法预防或纠正透明软骨退化、软骨下骨板增厚、骨赘形成或骨关节炎膝关节的机械功能障碍。
Zotero 插件
