Andersen Camilla, Walters Marie, Bundgaard Louise, Berg Lise Charlotte, Vonk Lucienne Angela, Lundgren-Åkerlund Evy, Henriksen Betina Lyngfeldt, Lindegaard Casper, Skovgaard Kerstin, Jacobsen Stine
Department of Veterinary Clinical Sciences, Faculty of Health and Medical Sciences, University of Copenhagen, Taastrup, Denmark.
Xintela AB, Lund, Sweden.
Front Vet Sci. 2024 Mar 26;11:1374681. doi: 10.3389/fvets.2024.1374681. eCollection 2024.
Osteoarthritis (OA) remains a major cause of lameness in horses, which leads to lost days of training and early retirement. Still, the underlying pathological processes are poorly understood. MicroRNAs (miRNAs) are small non-coding RNAs that serve as regulators of many biological processes including OA. Analysis of miRNA expression in diseased joint tissues such as cartilage and synovial membrane may help to elucidate OA pathology. Since integrin α10β1-selected mesenchymal stem cell (integrin α10-MSC) have shown mitigating effect on equine OA we here investigated the effect of integrin α10-MSCs on miRNA expression. Cartilage and synovial membrane was harvested from the middle carpal joint of horses with experimentally induced, untreated OA, horses with experimentally induced OA treated with allogeneic adipose-derived MSCs selected for the marker integrin α10-MSCs, and from healthy control joints. miRNA expression in cartilage and synovial membrane was established by quantifying 70 pre-determined miRNAs by qPCR. Differential expression of the miRNAs was evaluated by comparing untreated OA and control, untreated OA and MSC-treated OA, and joints with high and low pathology score. A total of 60 miRNAs were successfully quantified in the cartilage samples and 55 miRNAs were quantified in the synovial membrane samples. In cartilage, miR-146a, miR-150 and miR-409 had significantly higher expression in untreated OA joints than in control joints. Expression of miR-125a-3p, miR-150, miR-200c, and miR-499-5p was significantly reduced in cartilage from MSC-treated OA joints compared to the untreated OA joints. Expression of miR-139-5p, miR-150, miR-182-5p, miR-200a, miR-378, miR-409-3p, and miR-7177b in articular cartilage reflected pathology score. Several of these miRNAs are known from research in human patients with OA and from murine OA models. Our study shows that these miRNAs are also differentially expressed in experimental equine OA, and that expression depends on OA severity. Moreover, MSC treatment, which resulted in less severe OA, also affected miRNA expression in cartilage.
骨关节炎(OA)仍是马匹跛行的主要原因,会导致训练天数减少和提前退役。然而,其潜在的病理过程仍知之甚少。微小RNA(miRNA)是一类小的非编码RNA,可作为包括OA在内的许多生物过程的调节因子。分析患病关节组织(如软骨和滑膜)中的miRNA表达可能有助于阐明OA的病理学机制。由于整合素α10β1选择的间充质干细胞(整合素α10-MSC)已显示出对马OA的缓解作用,因此我们在此研究了整合素α10-MSC对miRNA表达的影响。从患有实验性诱导的未治疗OA的马、用选择整合素α10标记的同种异体脂肪来源的间充质干细胞治疗的实验性诱导OA的马以及健康对照关节的腕中关节采集软骨和滑膜。通过qPCR对70种预先确定的miRNA进行定量,从而确定软骨和滑膜中的miRNA表达。通过比较未治疗的OA与对照、未治疗的OA与MSC治疗的OA以及病理评分高和低的关节,评估miRNA的差异表达。在软骨样本中成功定量了总共60种miRNA,在滑膜样本中定量了55种miRNA。在软骨中,miR-146a、miR-150和miR-409在未治疗的OA关节中的表达明显高于对照关节。与未治疗的OA关节相比,MSC治疗的OA关节软骨中miR-125a-3p、miR-150、miR-200c和miR-499-5p的表达明显降低。关节软骨中miR-139-5p、miR-150、miR-182-5p、miR-200a、miR-378、miR-409-3p和miR-7177b的表达反映了病理评分。这些miRNA中的几种已在人类OA患者和小鼠OA模型的研究中有所报道。我们的研究表明,这些miRNA在实验性马OA中也存在差异表达,且表达取决于OA的严重程度。此外,导致OA不太严重的MSC治疗也影响了软骨中的miRNA表达。
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