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Peripheral T lymphocytes from patients with early systemic sclerosis co-cultured with autologous fibroblasts undergo an oligoclonal expansion similar to that occurring in the skin

机译:与自体成纤维细胞共培养的早期系统性硬化症患者的外周血T淋巴细胞的寡克隆扩增与皮肤中的类似

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摘要

In recent years several reports have suggested that T cells may have a role in systemic sclerosis (SSc). The aim of our study was to investigate the dynamics of T cell repertoire in early SSc disease analysing a target organ, the skin, and the peripheral blood. To date, indeed, it is not clear if T cell expansions found in SSc reflect a general activation or result from specific antigen stimulation in the target organs. This is an important point to assess in order to characterize the role of T cells in the development of SSc. To address these questions we studied T cell repertoire by CDR3 length analysis in skin biopsies and peripheral blood obtained from patients affected by SSc and we found that a skewed T cell repertoire was present only in the biopsies. In order to characterize more effectively the meaning of these data, we performed co-cultures using fibroblasts and peripheral blood mononuclear cells (PBMCs) obtained from SSc patients. These experiments showed that same T cell expansions were detectable in the skin of SSc patients and in the cultures of PBMCs and autologous fibroblasts of the patients but not in their peripheral blood. Taken together, these data suggest that fibroblasts trigger specific T cell expansions in the early phase of SSc.
机译:近年来,一些报道表明T细胞可能在系统性硬化症(SSc)中起作用。我们研究的目的是研究早期SSc疾病中T细胞库的动态,分析靶器官,皮肤和外周血。到目前为止,实际上,尚不清楚在SSc中发现的T细胞扩增是否反映了一般的激活或是由靶器官中特异性抗原刺激引起的。为了表征T细胞在SSc发育中的作用,评估这一点很重要。为了解决这些问题,我们通过从受SSc影响的患者获得的皮肤活检和外周血中的CDR3长度分析研究了T细胞库,我们发现仅在活检中存在偏斜的T细胞库。为了更有效地表征这些数据的含义,我们使用了成纤维细胞和从SSc患者获得的外周血单核细胞(PBMC)进行了共培养。这些实验表明,在SSc患者的皮肤以及患者的PBMC和自体成纤维细胞的培养物中可检测到相同的T细胞扩增,但在其外周血中未检测到。综上所述,这些数据表明成纤维细胞在SSc的早期触发了特定的T细胞扩增。

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