Evidence in support of the bone marrow as the primary lesion in axial spondyloarthritis.

IF 5.2 2区 医学 Q1 RHEUMATOLOGY
Walter P Maksymowych
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引用次数: 1

Abstract

Purpose of review: Over the past several decades, the concept that the primary lesion accounting for the development of axSpA is an enthesopathy has been widely accepted. However, the hallmark abnormality of axSpA occurs in the sacroiliac joint at the interface of cartilage and bone at a location remote from any anatomical enthesis. Both imaging and histopathological data from the sacroiliac joint point to immunopathogenetic events in the bone marrow as being of primary importance. Here, we discuss new developments in our understanding of immune events in the bone marrow relevant to axSpA that reinforce the need for a change in our conceptual paradigm for the pathogenesis of axSpA.

Recent findings: Human spinal enthesis samples contain myeloperoxidase-expressing cells, a marker of neutrophils, and mucosal-associated invariant T cells in the perientheseal bone marrow, which may be activated by stromal cells and circulating microbial products to express IL-17A and IL-17F and tumor necrosis factor (TNF). Evaluation of transcriptomes of monocytes from patients with axSpA demonstrates a lipopolysaccharide/TNF signature characterized by the expression of genes associated with granulocytopoietic bone marrow cells. This neutrophil-like phenotype is more evident in established and more severe axSpA and may be activated by microbial products from the gut. A similar expansion of granulocyte-monocyte progenitor-driven hematopoiesis occurs in the SKG mouse driven by granulocyte-macrophage colony-stimulating factor. Mesenchymal stem cells (MSCs) from ankylosing spondylitis patients are more likely to exhibit osteogenic differentiation than MSCs from healthy donors, which may be mediated by the formation of specific clusters of transcriptional factors, super enhancers, regulated by axSpA-associated single nucleotide polymorphisms located mostly in noncoding regions. TNF-α may enhance directional migration of AS-MSC compared with MSC from healthy controls from the bone marrow to entheseal soft tissue, which is mediated by increased expression of engulfment and cell motility protein 1 (ELMO1). TNF and IL-17A display differential effects on adipogenesis and osteogenesis of MSC in perientheseal bone marrow and soft tissue.

Summary: Bone marrow has the capacity to undergo rapid adaptation in terms of cell composition, differentiation, and immune function, resulting in inflammation and osteogenesis in axSpA.

支持骨髓作为轴性脊柱炎原发病变的证据。
综述目的:在过去的几十年里,导致axSpA发展的原发病变是一种终末期病变的概念已被广泛接受。然而,axSpA的标志性异常发生在骶髂关节软骨和骨的交界处,远离任何解剖端骨。骶髂关节的影像学和组织病理学资料都指出骨髓中的免疫发病事件是最重要的。在这里,我们讨论了我们对与axSpA相关的骨髓免疫事件的理解的新进展,这些进展加强了我们对axSpA发病机制的概念范式的改变。最近的发现:人脊髓终端标本中含有表达髓过氧化物酶的细胞(一种中性粒细胞的标记物),以及骨骺周骨髓中与粘膜相关的不变性T细胞,它们可能被基质细胞和循环微生物产物激活,表达IL-17A和IL-17F以及肿瘤坏死因子(TNF)。对axSpA患者单核细胞转录组的评估显示,与粒细胞生成骨髓细胞相关的基因表达具有脂多糖/TNF特征。这种中性粒细胞样表型在已建立的和更严重的axSpA中更为明显,并可能被肠道微生物产物激活。在粒细胞-巨噬细胞集落刺激因子驱动的SKG小鼠中,粒细胞-单核细胞祖细胞驱动的造血功能也出现了类似的扩增。来自强直性脊柱炎患者的间充质干细胞(MSCs)比来自健康供体的MSCs更有可能表现出成骨分化,这可能是由特定转录因子簇的形成介导的,超级增强子由位于非编码区的axspa相关单核苷酸多态性调控。与健康对照的骨髓间充质干细胞相比,TNF-α可能通过增加吞噬和细胞运动蛋白1 (ELMO1)的表达介导AS-MSC从骨髓向内脏软组织的定向迁移。TNF和IL-17A对骨骺周骨髓和软组织间充质干细胞的成脂和成骨有不同的影响。总结:在axSpA中,骨髓在细胞组成、分化和免疫功能方面具有快速适应的能力,导致炎症和成骨。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Current opinion in rheumatology
Current opinion in rheumatology 医学-风湿病学
CiteScore
9.70
自引率
2.00%
发文量
89
审稿时长
6-12 weeks
期刊介绍: A high impact review journal which boasts an international readership, Current Opinion in Rheumatology offers a broad-based perspective on the most recent and exciting developments within the field of rheumatology. Published bimonthly, each issue features insightful editorials and high quality invited reviews covering two or three key disciplines which include vasculitis syndromes, medical physiology and rheumatic diseases, crystal deposition diseases and rheumatoid arthritis. Each discipline introduces world renowned guest editors to ensure the journal is at the forefront of knowledge development and delivers balanced, expert assessments of advances from the previous year.
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