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类风湿关节炎、脊柱关节炎和强直性脊柱炎中的骨髓间充质干细胞:问题而非解决方案?

Bone marrow mesenchymal stem cells in rheumatoid arthritis, spondyloarthritis, and ankylosing spondylitis: problems rather than solutions?

机构信息

Centre Hospitalier Universitaire de Nantes, Nantes, France.

出版信息

Arthritis Res Ther. 2019 Nov 13;21(1):239. doi: 10.1186/s13075-019-2014-8.

Abstract

BACKGROUND

Bone marrow mesenchymal stem cells (BM-MSCs) can dampen inflammation in animal models of inflammatory rheumatisms and human osteoarthritis. They are expected to be a solution for numerous human conditions. However, in rheumatoid arthritis (RA) and spondyloarthritis (SpA), subsets of subchondral BM-MSCs might conversely fuel synovitis and enthesitis.

MAIN TEXT

Abnormal behaviour of BM-MSCs and/or their progeny has been found in RA and SpA. BM-MSCs also contribute to the ossifying processes observed in ankylosing spondylitis. Some synovial fibroblastic stem cells probably derive from BM-MSCs, but some stem cells can also migrate through the bare zone area of joints, not covered by cartilage, into the synovium. BM-MSCs can also migrate in the synovium over tendons. Sub-populations of bone marrow stem cells also invade the soft tissue side of enthesis via small holes in the bone cortex. The present review aims (1) to make a focus on these two aspects and (2) to put forward the hypothesis that lasting epigenetic changes of some BM-MSCs, induced by transient infections of the bone marrow close to the synovium and/or entheses (i.e. trained immunity of BM-MSCs and/or their progeny), contribute to the pathogenesis of inflammatory rheumatisms. Such hypothesis would fit with (1) the uneven distribution and/or flares of arthritis and enthesitis observed at the individual level in RA and SpA (reminiscent of what is observed following reactive arthritis and/or in Whipple's disease); (2) the subchondral bone marrow oedema and erosions occurring in many RA patients, in the bare zone area; and (3) the frequent relapses of RA and SpA despite bone marrow transplantation, whereas most BM-MSCs resist graft preconditioning.

CONCLUSION

Some BM-MSCs might be more the problem than the solution in inflammatory rheumatisms. Subchondral bone marrow BM-MSCs and their progeny trafficking through the bare zone area of joints or holes in the bone cortex of entheses should be thoroughly studied in RA and SpA respectively. This may be done first in animal models. Mini-arthroscopy of joints could also be used in humans to specifically sample tissues close to the bare zone and/or enthesis areas.

摘要

背景

骨髓间充质干细胞(BM-MSCs)可减轻炎症性风湿病和人类骨关节炎动物模型中的炎症。它们有望成为众多人类疾病的解决方案。然而,在类风湿关节炎(RA)和脊柱关节炎(SpA)中,软骨下 BM-MSCs 的亚群可能反而会加剧滑膜炎和附着点炎。

主要文本

已经在 RA 和 SpA 中发现 BM-MSCs 和/或其祖细胞的异常行为。BM-MSCs 也有助于强直性脊柱炎中观察到的骨化过程。一些滑膜成纤维干细胞可能来自 BM-MSCs,但一些干细胞也可以通过关节软骨下的裸露区(未被软骨覆盖)迁移到滑膜中。BM-MSCs 也可以在肌腱上的滑膜中迁移。骨髓干细胞的亚群也可以通过骨皮质上的小孔侵犯附着点的软组织侧。本综述旨在(1)重点关注这两个方面,(2)提出假设,即由靠近滑膜和/或附着点的骨髓短暂感染诱导的一些 BM-MSCs 的持久表观遗传变化(即 BM-MSCs 和/或其祖细胞的训练免疫),有助于炎症性风湿病的发病机制。这种假设与(1)RA 和 SpA 个体水平观察到的关节炎和附着点炎的不均匀分布和/或发作(类似于反应性关节炎和/或 Whipple 病后观察到的)一致;(2)许多 RA 患者在裸露区发生的软骨下骨髓水肿和侵蚀;(3)尽管进行了骨髓移植,但 RA 和 SpA 仍经常复发,而大多数 BM-MSCs 抵抗移植物预处理。

结论

在炎症性风湿病中,一些 BM-MSCs 可能是问题的根源,而不是解决方案。应分别在 RA 和 SpA 中深入研究通过关节裸露区或附着点骨皮质孔的软骨下骨髓 BM-MSCs 和其祖细胞的迁移。这可以首先在动物模型中进行。关节微型关节镜检查也可用于人类,以专门采集靠近裸露区和/或附着点区域的组织。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa3a/6854713/ff13e026ec4d/13075_2019_2014_Fig1_HTML.jpg

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