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整合素 α10β1 阳性间充质干细胞减轻马跗骨撞击模型中骨关节炎的进展。

Integrin α10β1-Selected Mesenchymal Stem Cells Mitigate the Progression of Osteoarthritis in an Equine Talar Impact Model.

机构信息

Cornell University, Ithaca, New York, USA.

Xintela AB, Medicon Village, Lund, Sweden.

出版信息

Am J Sports Med. 2020 Mar;48(3):612-623. doi: 10.1177/0363546519899087. Epub 2020 Jan 31.

Abstract

BACKGROUND

Early intervention with mesenchymal stem cells (MSCs) after articular trauma has the potential to limit progression of focal lesions and prevent ongoing cartilage degeneration by modulating the joint environment and/or contributing to repair. Integrin α10β1 is the main collagen type II binding receptor on chondrocytes, and MSCs that are selected for high expression of the α10 subunit have improved chondrogenic potential. The ability of α10β1-selected (integrin α10) MSCs to protect cartilage after injury has not been investigated.

PURPOSE

To investigate integrin α10 MSCs to prevent posttraumatic osteoarthritis in an equine model of impact-induced talar injury.

STUDY DESIGN

Controlled laboratory study.

METHODS

Focal cartilage injuries were created on the tali of horses (2-5 years, n = 8) by using an impacting device equipped to measure impact stress. Joints were treated with 20 × 10 allogenic adipose-derived α10 MSCs or saline vehicle (control) 4 days after injury. Synovial fluid was collected serially and analyzed for protein content, cell counts, markers of inflammation (prostaglandin E2, tumor necrosis factor α) and collagen homeostasis (procollagen II C-propeptide, collagen type II cleavage product), and glycosaminoglycan content. Second-look arthroscopy was performed at 6 weeks, and horses were euthanized at 6 months. Joints were imaged with radiographs and quantitative 3-T magnetic resonance imaging. Postmortem examinations were performed, and India ink was applied to the talar articular surface to identify areas of cartilage fibrillation. Synovial membrane and osteochondral histology was performed, and immunohistochemistry was used to assess type I and II collagen and lubricin. A mixed effect model with Tukey post hoc and linear contrasts or paired tests were used, as appropriate.

RESULTS

Integrin α10 MSC-treated joints had less subchondral bone sclerosis on radiographs ( = .04) and histology ( = .006) and less cartilage fibrillation ( = .04) as compared with control joints. On gross pathology, less India ink adhered to impact sites in treated joints than in controls, which may be explained by the finding of more prominent lubricin immunostaining in treated joints. Prostaglandin E2 concentration in synovial fluid and mononuclear cell synovial infiltrate were increased in treated joints, suggesting possible immunomodulation by integrin α10 MSCs.

CONCLUSION

Intra-articular administration of integrin α10 MSCs is safe, and evidence suggests that the cells mitigate the effects of joint trauma.

CLINICAL RELEVANCE

This preclinical study indicates that intra-articular therapy with integrin α10 MSCs after joint trauma may be protective against posttraumatic osteoarthritis.

摘要

背景

关节创伤后早期干预间充质干细胞(MSCs)有可能通过调节关节环境和/或促进修复来限制局灶性病变的进展并防止持续的软骨退化。整合素 α10β1 是软骨细胞中主要的 II 型胶原结合受体,选择高表达 α10 亚基的 MSC 具有改善的软骨生成潜力。尚未研究过 α10β1 选择(整合素 α10)MSC 在受伤后保护软骨的能力。

目的

在撞击诱导距骨损伤的马模型中,研究整合素 α10 MSC 预防创伤后骨关节炎。

研究设计

对照实验室研究。

方法

使用配备有测量冲击应力的设备的撞击装置在马的距骨上创建局灶性软骨损伤(2-5 岁,n=8)。在受伤后 4 天,关节用 20×10 个同种异体脂肪衍生的 α10 MSC 或盐水载体(对照)进行治疗。连续采集滑液进行分析,以测定蛋白含量、细胞计数、炎症标志物(前列腺素 E2、肿瘤坏死因子-α)和胶原稳态(原胶原 II C-前肽、II 型胶原裂解产物)以及糖胺聚糖含量。6 周时进行二次关节镜检查,6 个月时处死马。使用 X 线和定量 3-T 磁共振成像对关节进行成像。进行尸检,并在距骨关节表面涂抹印度墨水以识别软骨纤颤区域。进行滑膜和骨软骨组织学检查,并进行 I 型和 II 型胶原和润滑素的免疫组化。使用混合效应模型进行 Tukey 事后检验和线性对比或配对 t 检验,具体取决于情况。

结果

与对照组相比,整合素 α10 MSC 治疗的关节在 X 线( =.04)和组织学( =.006)上的软骨下骨硬化程度较低,并且软骨纤颤程度较低( =.04)。大体病理学上,治疗关节中附着在撞击部位的印度墨水较少,这可能是由于治疗关节中润滑素免疫染色更明显所致。滑液中的前列腺素 E2 浓度和单核细胞滑膜浸润在治疗关节中增加,这表明整合素 α10 MSC 可能具有免疫调节作用。

结论

关节内给予整合素 α10 MSC 是安全的,并且有证据表明细胞减轻了关节创伤的影响。

临床相关性

这项临床前研究表明,关节创伤后关节内给予整合素 α10 MSC 可能对创伤后骨关节炎具有保护作用。

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