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Identification of microRNA-221/222 and microRNA-323-3p association with rheumatoid arthritis via predictions using the human tumour necrosis factor transgenic mouse model.

机译：通过使用人类肿瘤坏死因子转基因小鼠模型的预测，鉴定与风湿性关节炎相关的microRNA-221 / 222和microRNA-323-3p。

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OBJECTIVE: To identify novel microRNA (miR) associations in synovial fibroblasts (SF), by performing miR expression profiling on cells isolated from the human tumour necrosis factor (TNF) transgenic mouse model (TghuTNF, Tg197) and patients biopsies. METHODS: miR expression in SF from TghuTNF and wild-type (WT) control mice were determined by miR deep sequencing (miR-seq) and the arthritic profile was established by pairwise comparisons. Quantitative PCR analysis was utilised for profile validation, miR and gene quantitation in patient SF. Dysregulated miR target genes and pathways were predicted via bioinformatic algorithms and validated using gain-of-function coupled with reporter assay experiments. RESULTS: miR-seq demonstrated that TghuTNF-SF exhibit a distinct pathogenic profile with 22 significantly upregulated and 30 significantly downregulated miR. Validation assays confirmed the dysregulation of miR-223, miR-146a and miR-155 previously associated with human rheumatoid arthritis (RA) pathology, as well as that of miR-221/222 and miR-323-3p. Notably, the latter were also found significantly upregulated in patient RA SF, suggesting for the first time their association with RA pathology. Bioinformatic analysis suggested Wnt/cadherin signalling as a putative pathway target. miR-323-3p overexpression was shown to enhance Wnt pathway activation and decrease the levels of its predicted target β-transducin repeat containing, an inhibitor of β-catenin. CONCLUSIONS: Using miR-seq-based profiling in SF from the TghuTNF mouse model and validations in RA patient biopsies, the authors identified miR-221/222 and miR-323-3p as novel dysregulated miR in RA SF. Furthermore, the authors show that miR-323-3p is a positive regulator of WNT/cadherin signalling in RA SF suggesting its potential pathogenic involvement and future use as a therapeutic target in RA.

机译：目的：通过对分离自人类肿瘤坏死因子（TNF）转基因小鼠模型（TghuTNF，Tg197）和患者活检组织的细胞进行miR表达谱分析，以鉴定滑膜成纤维细胞（SF）中的新型microRNA（miR）关联。方法：通过miR深度测序（miR-seq）测定TghuTNF和野生型（WT）对照小鼠的SF中的miR表达，并通过成对比较建立关节炎特征。定量PCR分析用于患者SF的谱图验证，miR和基因定量。通过生物信息学算法预测失调的miR靶基因和途径，并通过功能获得和报告基因检测实验进行验证。结果：miR-seq证实TghuTNF-SF表现出独特的致病性，其中miR显着上调22个，而miR显着下调30个。验证分析证实了先前与人类类风湿性关节炎（RA）病理相关的miR-223，miR-146a和miR-155失调，以及miR-221 / 222和miR-323-3p失调。值得注意的是，后者在患者RA SF中也被显着上调，这首次表明它们与RA病理学相关。生物信息学分析表明Wnt / cadherin信号作为推定的通路靶标。显示miR-323-3p过表达可增强Wnt途径活化并降低其预测的目标β-转导蛋白重复序列（β-catenin抑制剂）的水平。结论：使用来自TghuTNF小鼠模型的SF中基于miR-seq的分析以及在RA患者活检中的验证，作者确定了miR-221 / 222和miR-323-3p是RA SF中新失调的miR。此外，作者表明，miR-323-3p是RA SF中WNT /钙黏着蛋白信号转导的正调节剂，表明其潜在的病原体参与和将来在RA中的治疗靶标。

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Pandis, I; Ospelt, C; Karagianni, N; Denis, MC; Reczko, M; Camps, C; Hatzigeorgiou, AG; Ragoussis, J; Gay, S; Kollias, G;
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1. Identification of microRNA-221/222 and microRNA-323-3p association with rheumatoid arthritis via predictions using the human tumour necrosis factor transgenic mouse model [J] . PandisI., OspeltC., KaragianniN., Annals of the Rheumatic Diseases: A Journal of Clinical Rheumatology and Connective Tissue Research . 2012 ,第10期

机译：通过使用人类肿瘤坏死因子转基因小鼠模型的预测鉴定与风湿性关节炎相关的microRNA-221 / 222和microRNA-323-3p
2. Association of microRNA-221/222 and -323-3p with rheumatoid arthritis via predictions using the human TNF transgenic mouse model [J] . Ioannis Pandis, Caroline Ospelt, Niki Karagianni, Arthritis Research . 2012 ,第Suppla1期

机译：通过使用人类TNF转基因小鼠模型的预测，将microRNA-221 / 222和-323-3p与类风湿性关节炎相关联
3. Polymorphisms within the human leucocyte antigen-E gene and their associations with susceptibility to rheumatoid arthritis as well as clinical outcome of anti-tumour necrosis factor therapy [J] . Iwaszko M., Swierkot J., Kolossa K., Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology . 2015 ,第3期

机译：人白细胞抗原-E基因内的多态性及其与类风湿性关节炎易感性的关联以及抗肿瘤坏死因子疗法的临床结果
4. Identification and Characterization of Novel Autoantibody Biomarkcrs for Rheumatoid Factor-Negative and Accp- Negative Rheumatoid Arthritis [C] . Anh Nguyen-Hung, Binh Le-Thanh, Cindy Govart International Confernece on Biomedical Engineering in Vietnam . 2013

机译：用于类风湿性因子阴性和ACCP阴性类风湿性关节炎的新型自身抗体BIOMAKCR的鉴定与表征
5. Pro-inflammatory T helper cells in rheumatoid arthritis: Influence of tumour necrosis factor inhibition. [D] . Aerts, Nicolaas. 2010

机译：类风湿关节炎中的促炎性T辅助细胞：肿瘤坏死因子抑制的影响。
6. Association of microRNA-221/222 and -323-3p with rheumatoid arthritis via predictions using the human TNF transgenic mouse model [O] . Ioannis Pandis, Caroline Ospelt, Niki Karagianni, 2012

机译：通过使用人类TNF转基因小鼠模型的预测将microRNA-221 / 222和-323-3p与类风湿性关节炎相关联
7. Identification of microRNA-221/222 and microRNA-323-3p association with rheumatoid arthritis via predictions using the human tumour necrosis factor transgenic mouse model [O] . Pandis, Ioannis, Ospelt, Caroline, Karagianni, Niki, 2012

机译：通过使用人类肿瘤坏死因子转基因小鼠模型的预测鉴定与风湿性关节炎相关的microRNA-221 / 222和microRNA-323-3p

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Identification of microRNA-221/222 and microRNA-323-3p association with rheumatoid arthritis via predictions using the human tumour necrosis factor transgenic mouse model.

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