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粘弹性补充剂可能会在骨关节炎中保留胫骨软骨和胶原蛋白:来自骨关节炎临床前模型的研究结果。

Viscosupplementation may preserve tibial cartilage and collagen in osteoarthritis: findings from a preclinical model of osteoarthritis.

作者信息

Lokhnauth John, Driscoll Kevin E, Bendele Alison, Niazi Faizan, Liang Alfred, Larsen Crilles C

机构信息

Ferring Pharmaceuticals Inc., 100 Interpace Parkway, Parsippany, NJ, 07054, USA.

Healthcare Innovation Partners, Mountain Lakes, NJ, USA.

出版信息

J Exp Orthop. 2020 May 31;7(1):39. doi: 10.1186/s40634-020-00256-4.

Abstract

PURPOSE

Intraarticular (IA) hyaluronic acid (HA) injection is used to reduce pain and improve mobility in knee osteoarthritis (OA). Little is known about histopathological changes underlying HA efficacy. This study investigated dose-related effects of 1% sodium hyaluronate (BioHA) on knee joint histopathology and pain responses in a medial meniscal tear (MMT) rat model of OA.

METHODS

Following MMT surgery, rats were randomized into treatment groups: single IA injection of vehicle, BioHA, or an avian-derived hyaluronic acid (hylan G-F 20) on Day 7; or 3 weekly injections of vehicle or BioHA on Days 7, 14, and 21. On Day 35, joints were evaluated by microscopic histopathology for cartilage degeneration, collagen degeneration, synovitis, and cytokine expression (tumor necrosis factor α, transforming growth factor β).

RESULTS

Joint pathology for control animals was consistent with that expected for the MMT model. Rats treated with 3 injections of IA-BioHA had significantly reduced collagen degeneration (21%) relative to control animals. No significant change in collagen degeneration was observed for rats given a single injection of hylan G-F 20 or IA-BioHA compared to control animals. HA treatment did not affect cytokine expression.

CONCLUSIONS

IA-BioHA viscosupplementation in a rat MMT model of OA showed preservation of joint cartilage and collagen. This effect was most pronounced on tibial surfaces having less severe injury, suggesting that treatment should be initiated early in the disease process. A comparison of responses to IA-BioHA or hylan G-F 20 in the MMT rat OA model suggest IA-BioHA may be more effective in preserving joint connective tissue.

摘要

目的

关节内(IA)注射透明质酸(HA)用于减轻膝关节骨关节炎(OA)的疼痛并改善关节活动度。关于HA疗效背后的组织病理学变化知之甚少。本研究在OA的内侧半月板撕裂(MMT)大鼠模型中,研究了1%透明质酸钠(BioHA)对膝关节组织病理学和疼痛反应的剂量相关影响。

方法

MMT手术后,大鼠被随机分为治疗组:在第7天单次关节内注射赋形剂、BioHA或禽源透明质酸(hylan G-F 20);或在第7天、14天和21天每周注射3次赋形剂或BioHA。在第35天,通过显微镜组织病理学评估关节的软骨退变、胶原退变、滑膜炎和细胞因子表达(肿瘤坏死因子α、转化生长因子β)。

结果

对照动物的关节病理学与MMT模型预期一致。与对照动物相比,接受3次关节内注射IA-BioHA治疗的大鼠胶原退变显著减少(21%)。与对照动物相比,单次注射hylan G-F 20或IA-BioHA的大鼠胶原退变未见显著变化。HA治疗不影响细胞因子表达。

结论

在大鼠MMT OA模型中,IA-BioHA关节腔内补充显示出对关节软骨和胶原的保护作用。这种作用在损伤较轻的胫骨表面最为明显,提示应在疾病早期开始治疗。MMT大鼠OA模型中对IA-BioHA或hylan G-F 20反应的比较表明,IA-BioHA在保护关节结缔组织方面可能更有效。

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