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与正常关节相比,来源于犬骨关节炎关节的滑膜膜源性间充质祖细胞具有较低的软骨生成能力和较高的成骨能力。

Synovial membrane-derived mesenchymal progenitor cells from osteoarthritic joints in dogs possess lower chondrogenic-, and higher osteogenic capacity compared to normal joints.

机构信息

Department of Clinical Sciences, Faculty of Veterinary Medicine, Utrecht University, Utrecht, The Netherlands.

Department of Orthopaedics and Sports Medicine, Erasmus MC, University Medical Center Rotterdam, Rotterdam, The Netherlands.

出版信息

Stem Cell Res Ther. 2022 Sep 5;13(1):457. doi: 10.1186/s13287-022-03144-z.

Abstract

BACKGROUND

Synovial membrane-derived mesenchymal progenitor cells (SM-MPCs) are a promising candidate for the cell-based treatment of osteoarthritis (OA) considering their in vitro and in vivo capacity for cartilage repair. However, the OA environment may adversely impact their regenerative capacity. There are no studies for canine (c)SM-MPCs that compare normal to OA SM-MPCs, even though dogs are considered a relevant animal model for OA. Therefore, this study compared cSM-MPCs from normal and OA synovial membrane tissue to elucidate the effect of the OA environment on MPC numbers, indicated by CD marker profile and colony-forming unit (CFU) capacity, and the impact of the OA niche on tri-lineage differentiation.

METHODS

Normal and OA synovial membrane were collected from the knee joints of healthy dogs and dogs with rupture of the cruciate ligaments. The synovium was assessed by histopathological OARSI scoring and by RT-qPCR for inflammation/synovitis-related markers. The presence of cSM-MPCs in the native tissue was further characterized with flow cytometry, RT-qPCR, and immunohistochemistry, using the MPC markers; CD90, CD73, CD44, CD271, and CD34. Furthermore, cells isolated upon enzymatic digestion were characterized by CFU capacity, and a population doublings assay. cSM-MPCs were selected based on plastic adherence, expanded to passage 2, and evaluated for the expression of MPC-related surface markers and tri-lineage differentiation capacity.

RESULTS

Synovial tissue collected from the OA joints had a significantly higher OARSI score compared to normal joints, and significantly upregulated inflammation/synovitis markers S100A8/9, IL6, IL8, and CCL2. Both normal and OA synovial membrane contained cells displaying MPC properties, including a fibroblast-like morphology, CFU capacity, and maintained MPC marker expression over time during expansion. However, OA cSM-MPCs were unable to differentiate towards the chondrogenic lineage and had low adipogenic capacity in contrast to normal cSM-MPCs, whereas they possessed a higher osteogenic capacity. Furthermore, the OA synovial membrane contained significantly lower percentages of CD90+, CD44+, CD34+, and CD271+ cells.

CONCLUSIONS

The OA environment had adverse effects on the regenerative potential of cSM-MPCs, corroborated by decreased CFU, population doubling, and chondrogenic capacity compared to normal cSM-MPCs. OA cSM-MPCs may be a less optimal candidate for the cell-based treatment of OA than normal cSM-MPCs.

摘要

背景

滑膜膜源性间充质祖细胞(SM-MPCs)具有体外和体内软骨修复能力,是治疗骨关节炎(OA)的细胞治疗有希望的候选物。然而,OA 环境可能会对其再生能力产生不利影响。尽管狗被认为是 OA 的相关动物模型,但没有关于犬(c)SM-MPCs 的研究比较正常与 OA SM-MPCs。因此,本研究比较了来自正常和 OA 滑膜组织的 cSM-MPCs,以阐明 OA 环境对 MPC 数量的影响,通过 CD 标志物谱和集落形成单位(CFU)能力来表示,并探讨 OA 生态位对三系分化的影响。

方法

从健康狗和十字韧带断裂狗的膝关节中收集正常和 OA 滑膜。通过组织病理学 OARSI 评分和 RT-qPCR 评估滑膜炎症/滑膜炎相关标志物。使用 MPC 标志物 CD90、CD73、CD44、CD271 和 CD34 进一步对天然组织中的 cSM-MPCs 进行流式细胞术、RT-qPCR 和免疫组织化学分析。此外,通过 CFU 能力和群体倍增测定从酶消化分离的细胞进行了表征。基于塑料粘附选择 cSM-MPCs,传代 2 代,并评估与 MPC 相关的表面标志物表达和三系分化能力。

结果

与正常关节相比,OA 关节的滑膜组织 OARSI 评分显著升高,炎症/滑膜炎标志物 S100A8/9、IL6、IL8 和 CCL2 的表达显著上调。正常和 OA 滑膜均含有具有 MPC 特性的细胞,包括成纤维细胞样形态、CFU 能力,并在传代过程中随着时间的推移保持 MPC 标志物的表达。然而,OA cSM-MPC 无法向软骨谱系分化,与正常 cSM-MPC 相比,脂肪形成能力较低,而骨形成能力较高。此外,OA 滑膜中 CD90+、CD44+、CD34+和 CD271+细胞的百分比明显较低。

结论

OA 环境对 cSM-MPCs 的再生潜力产生了不利影响,与正常 cSM-MPCs 相比,CFU、倍增和软骨形成能力降低。OA cSM-MPCs 可能不如正常 cSM-MPCs 是 OA 细胞治疗的理想候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/732a/9446738/e3f5c63a30f4/13287_2022_3144_Fig1_HTML.jpg

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