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Beyond Autoantibodies: Biologic Roles of Human Autoreactive B Cells in Rheumatoid Arthritis Revealed by RNA‐Sequencing

机译:除了自身抗体之外:RNA测序揭示了类风湿性关节炎中人自身反应性B细胞的生物学作用

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Objective To obtain the comprehensive transcriptome profile of human citrulline‐specific B cells from patients with rheumatoid arthritis ( RA ). Methods Citrulline‐ and hemagglutinin‐specific B cells were sorted by flow cytometry using peptide–streptavidin conjugates from the peripheral blood of RA patients and healthy individuals. The transcriptome profile of the sorted cells was obtained by RNA ‐sequencing, and expression of key protein molecules was evaluated by aptamer‐based SOMA scan assay and flow cytometry. The ability of these proteins to effect differentiation of osteoclasts and proliferation and migration of synoviocytes was examined by in vitro functional assays. Results Citrulline‐specific B cells, in comparison to citrulline‐negative B cells, from patients with RA differentially expressed the interleukin‐15 receptor α ( IL ‐15Rα) gene as well as genes related to protein citrullination and cyclic AMP signaling. In analyses of an independent cohort of cyclic citrullinated peptide–seropositive RA patients, the expression of IL ‐15Rα protein was enriched in citrulline‐specific?B cells from the patients’ peripheral blood, and surprisingly, all B cells from RA patients were capable of producing the epidermal growth factor ligand amphiregulin ( AREG ). Production of AREG directly led to increased migration and proliferation of fibroblast‐like synoviocytes, and, in combination with anti–citrullinated protein antibodies, led to the increased differentiation of osteoclasts. Conclusion To the best of our knowledge, this is the first study to document the whole transcriptome profile of autoreactive B cells in any autoimmune disease. These data identify several genes and pathways that may be targeted by repurposing several US Food and Drug Administration–approved drugs, and could serve as the foundation for the comparative assessment of B cell profiles in other autoimmune diseases.
机译:目的了解类风湿性关节炎患者(RA)患者人瓜粉胺特异性B细胞的综合转录组型材。方法使用来自RA患者和健康个体的外周血的肽 - 链霉抗生物素蛋白缀合物的流式细胞仪对特异性B细胞对特异性酸素和血凝素的B细胞。通过RNA序列获得分选电池的转录组曲线,并通过基于适体的SOMA扫描测定和流式细胞术评估关键蛋白质分子的表达。通过体外功能测定检查这些蛋白质以分化骨细胞和增殖和迁移和迁移的能力。结果与瓜氨酸阴性B细胞相比,瓜氨酸特异性B细胞差异地表达了白细胞介素-15受体α(IL-15Rα)基因以及与蛋白质瓜氨酸和环状AMP信号相关的基因。在分析循环柑橘肽肽 - 血清阳性RA患者的独立队列中,IL-15Rα蛋白的表达在患者的外周血中富含瓜氨酸特异性的βb细胞,令人惊讶的是,来自RA患者的所有B细胞都有能力产生表皮生长因子配体amphegegulin(ARSG)。 ISG的生产直接导致成纤维细胞样Synoviocytes的迁移和增殖增加,并且与抗瓜氨酸蛋白抗体组合,导致了骨细胞的分化增加。结论据我们所知,这是第一次记录在任何自身免疫疾病中自身反应B细胞的整个转录组型的研究。这些数据鉴定了几种基因和途径,可以通过重新估算几种美国食品和药物管理批准的药物来靶向,并且可以作为对其他自身免疫疾病对B细胞谱的比较评估的基础。

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