Reactivation of NR4A1 Restrains Chondrocyte Inflammation and Ameliorates Osteoarthritis in Rats

Xiong, Yan; Ran, Jisheng; Xu, Langhai; Tong, Zhou; Abdo, Moqbel Safwat Adel; Ma, Chiyuan; Xu, Kai; He, Yuzhe; Wu, Zhipeng; Chen, Zhonggai; Hu, Pengfei; Jiang, Lifeng; Bao, Jiapeng; Chen, Weiping; Wu, Lidong

doi:10.3389/fcell.2020.00158

Cited by 31 publications

(25 citation statements)

References 46 publications

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“…Further, if the existence of cluster O3 is due to the osteoarthritis, specific markers NR4A1 and NR4A2, would have important roles in osteoarthritis pathogenesis. While previous studies have reported NR4A1 [ 80 ] and NR4A2 [ 81 ] to be regulators of inflammatory responses in chondrocytes, no study has proposed the relationship between osteoarthritis and NR4A1 produced by osteoblasts. In addition, scRNA-seq studies in both normal mouse osteoblasts in vivo performed by Tikhonova et al [ 17 ] and transcriptional profiles of mouse osteoblasts in vitro [ 76 ] showed the presence of NR4A1 in normal osteoblasts.…”

Section: Discussionmentioning

confidence: 99%

A systematic dissection of human primary osteoblasts in vivo at single-cell resolution

Gong

Yang

et al. 2021

Aging

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Human osteoblasts are multifunctional bone cells, which play essential roles in bone formation, angiogenesis regulation, as well as maintenance of hematopoiesis. However, the categorization of primary osteoblast subtypes in vivo in humans has not yet been achieved. Here, we used single-cell RNA sequencing (scRNA-seq) to perform a systematic cellular taxonomy dissection of freshly isolated human osteoblasts from one 31-year-old male with osteoarthritis and osteopenia after hip replacement. Based on the gene expression patterns and cell lineage reconstruction, we identified three distinct cell clusters including preosteoblasts, mature osteoblasts, and an undetermined rare osteoblast subpopulation. This novel subtype was found to be the major source of the nuclear receptor subfamily 4 group A member 1 and 2 (NR4A1 and NR4A2) in primary osteoblasts, and the expression of NR4A1 was confirmed by immunofluorescence staining on mouse osteoblasts in vivo . Trajectory inference analysis suggested that the undetermined cluster, together with the preosteoblasts, are involved in the regulation of osteoblastogenesis and also give rise to mature osteoblasts. Investigation of the biological processes and signaling pathways enriched in each subpopulation revealed that in addition to bone formation, preosteoblasts and undetermined osteoblasts may also regulate both angiogenesis and hemopoiesis. Finally, we demonstrated that there are systematic differences between the transcriptional profiles of human and mouse osteoblasts, highlighting the necessity for studying bone physiological processes in humans rather than solely relying on mouse models. Our findings provide novel insights into the cellular heterogeneity and potential biological functions of human primary osteoblasts at the single-cell level.

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Section: Discussionmentioning

confidence: 99%

A systematic dissection of human primary osteoblasts in vivo at single-cell resolution

Gong

Yang

et al. 2021

Aging

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“…NR4A1–NR4A3 expression is elevated in synovial tissue MSC and fibroblast-like stromal cells (FLSs), macrophage, endothelium, cartilage, and PGE2-stimulated chondrocytes from patients with RA, psoriatic arthritis, or osteoarthritis, making NR4A receptors attractive targets in rheumatic and skin diseases (McMorrow and Murphy, 2011 ; Marzaioli et al, 2012 ; Shi et al, 2017 ; Xiong et al, 2020 ). Stromal cell hyperplasia and development of a “tumor-like pannus” are characteristics of chronic inflammatory diseases including RA and psoriatic arthritis (Bottini and Firestein, 2013 ).…”

Section: (Vi) Nr4a1-nr4a3 Receptors In Rheumatic Diseasesmentioning

confidence: 99%

Targeting NR4A Nuclear Receptors to Control Stromal Cell Inflammation, Metabolism, Angiogenesis, and Tumorigenesis

Crean

Murphy

2021

Front. Cell Dev. Biol.

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The NR4A1–NR4A3 (Nur77, Nurr1, and Nor-1) subfamily of nuclear receptors is a group of immediate early genes induced by a pleiotropy of stimuli including peptide hormones, growth factors, cytokines, inflammatory, and physiological stimuli, and cellular stress. NR4A receptors function as potent sensors of changes in the cellular microenvironment to control physiological and pathological processes through genomic and non-genomic actions. NR4A receptors control metabolism and cardiovascular and neurological functions and mediate immune cell homeostasis in inflammation and cancer. This receptor subfamily is increasingly recognized as an important molecular connection between chronic inflammation, altered immune cell responses, and cancer development. In this review, we examine how transcriptome analysis identified NR4A1/NR4A2 receptors as transcriptional regulators in mesenchymal stromal cell (MSC) migration, cell cycle progression, and cytokine production to control local immune responses. In chronic inflammatory conditions, such as rheumatoid arthritis, NR4A receptors have been shown to modify the activity of MSC and fibroblast-like stromal cells to regulate synovial tissue hyperplasia, pathological angiogenesis, and cartilage turnover in vivo. Additionally, as NR4A1 has been observed as a major transcriptional regulator in tumor–stromal communication controlling tumorigenesis, we discuss how advances in the pharmacological control of these receptors lead to important new mechanistic insights into understanding the role of the tumor microenvironment in health and disease.

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“…7 NR4A1 expression levels were also found to be elevated in the joint tissues of patients with knee osteoarthritis, and a dysfunction due to phosphorylation was shown to contribute to the exacerbation of inflammation. 35 On the other hand, the expression levels of NR4A1 were decreased in the intestines of patients with ulcerative colitis and Crohn's disease, which is characterized by fibrosis in the colon, and the transcriptional activity of NR4A1 was decreased by SNPs in H3K27. 36 While the expression pattern of NR4A1 varies under different disease conditions, the loss-of-function of NR4A1 is commonly involved in their pathogenesis.…”

Section: Discussionmentioning

confidence: 99%

The role of nuclear receptor 4A1 (NR4A1) in drug‐induced gingival overgrowth

et al. 2021

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Drug‐induced gingival overgrowth (DIGO) is a side effect of cyclosporine A (CsA), nifedipine (NIF), and phenytoin (PHT). Nuclear receptor 4A1 (NR4A1) plays a role in fibrosis in multiple organs. However, the relationship between NR4A1 and DIGO remains unclear. We herein investigated the involvement of NR4A1 in DIGO. In the DIGO mouse model, CsA inhibited the up‐regulation of Nr4a1 expression induced by periodontal disease (PD) in gingival tissue, but not that of Col1a1 and Pai1. We detected gingival overgrowth (GO) in Nr4a1 knock out (KO) mice with PD. A NR4A1 agonist inhibited the development of GO in DIGO model mice. TGF‐β increased Col1a1 and Pai1 expression levels in KO mouse gingival fibroblasts (mGF) than in wild‐type mice, while the overexpression of NR4A1 in KO mGF suppressed the levels. NR4A1 expression levels in gingival tissue were significantly lower in DIGO patients than in PD patients. We also investigated the relationship between nuclear factor of activated T cells (NFAT) and NR4A1. NFATc3 siRNA suppressed the TGF‐β‐induced up‐regulation of NR4A1 mRNA expression in human gingival fibroblasts (hGF). CsA suppressed the TGF‐β‐induced translocation of NFATc3 into the nuclei of hGF. Furthermore, NIF and PHT also decreased NR4A1 mRNA expression levels and suppressed the translocation of NFATc3 in hGF. We confirmed that CsA, NIF, and PHT reduced cytosolic calcium levels increased by TGF‐β, while CaCl2 enhanced the TGF‐β‐up‐regulated NR4A1 expression. We propose that the suppression of the calcium‐NFATc3‐NR4A1 cascade by these three drugs plays a role in the development of DIGO.

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Reactivation of NR4A1 Restrains Chondrocyte Inflammation and Ameliorates Osteoarthritis in Rats

Cited by 31 publications

References 46 publications

A systematic dissection of human primary osteoblasts in vivo at single-cell resolution

A systematic dissection of human primary osteoblasts in vivo at single-cell resolution

Targeting NR4A Nuclear Receptors to Control Stromal Cell Inflammation, Metabolism, Angiogenesis, and Tumorigenesis

The role of nuclear receptor 4A1 (NR4A1) in drug‐induced gingival overgrowth

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