通过下一代测序对系统性红斑狼疮患者外周血T细胞受体多样性进行纵向分析。
Longitudinal analysis of peripheral blood T cell receptor diversity in patients with systemic lupus erythematosus by next-generation sequencing.
作者信息
Thapa Dharma R, Tonikian Raffi, Sun Chao, Liu Mei, Dearth Andrea, Petri Michelle, Pepin Francois, Emerson Ryan O, Ranger Ann
机构信息
Biogen, 250 Binney Street, Cambridge, MA, 02142, USA.
Novartis Pharmaceuticals Canada Inc, 385 Bouchard Boulevard, Dorval, QC, H9S 1A9, Canada.
出版信息
Arthritis Res Ther. 2015 May 23;17(1):132. doi: 10.1186/s13075-015-0655-9.
INTRODUCTION
T cells play an important role in the pathogenesis of systemic lupus erythematosus (SLE). Clonal expansion of T cells correlating with disease activity has been observed in peripheral blood (PB) of SLE subjects. Recently, next-generation sequencing (NGS) of the T cell receptor (TCR) β loci has emerged as a sensitive way to measure the T cell repertoire. In this study, we utilized NGS to assess whether changes in T cell repertoire diversity in PB of SLE patients correlate with or predict changes in disease activity.
METHODS
Total RNA was isolated from the PB of 11 SLE patients. Each subject had three samples, collected at periods of clinical quiescence and at a flare. Twelve age-matched healthy controls (HC) were used for reference. NGS was used to profile the complementarity-determining region 3 (CDR3) of the rearranged TCR β loci.
RESULTS
Relative to the HC, SLE patients (at quiescence) demonstrated a 2.2-fold reduction in repertoire diversity in a given PB volume (P <0.0002), a more uneven distribution of the repertoire (Gini coefficient, HC vs SLE, P = 0.015), and a trend toward increased percentage of expanded clones in the repertoire (clone size >1.0%, HC vs SLE, P = 0.078). No significant correlation between the overall repertoire diversity and clinical disease activity was observed for most SLE patients with only two of eleven SLE patients showing a decreasing trend in repertoire diversity approaching the flare time point. We did not observe any overlap of CDR3 amino acid sequences or a preferential Vβ or Jβ gene usage among the top 100 expanded clones from all SLE patients. In both HC and SLE, the majority of the expanded clones were remarkably stable over time (HC = 5.5 ±0.5 months, SLE = 7.2 ±2.4 months).
CONCLUSIONS
A significant decrease in T cell repertoire diversity was observed in PB of SLE patients compared to HC. However, in most SLE patients, repertoire diversity did not change significantly with increases in disease activity to a flare. Thus, without a priori knowledge of disease-specific clones, monitoring TCR repertoire in PB from SLE patients is not likely to be useful to predict changes in disease activity.
引言
T细胞在系统性红斑狼疮(SLE)的发病机制中起重要作用。在SLE患者的外周血(PB)中已观察到与疾病活动相关的T细胞克隆性扩增。最近,T细胞受体(TCR)β基因座的下一代测序(NGS)已成为一种测量T细胞库的灵敏方法。在本研究中,我们利用NGS评估SLE患者PB中T细胞库多样性的变化是否与疾病活动的变化相关或可预测疾病活动的变化。
方法
从11例SLE患者的PB中分离总RNA。每个受试者有三个样本,分别在临床静止期和病情发作时采集。使用12名年龄匹配的健康对照(HC)作为参照。NGS用于分析重排的TCRβ基因座的互补决定区3(CDR3)。
结果
相对于HC,SLE患者(静止期)在给定PB体积中的库多样性降低了2.2倍(P <0.0002),库的分布更不均匀(基尼系数,HC与SLE相比,P = 0.015),并且库中扩增克隆的百分比有增加趋势(克隆大小>1.0%,HC与SLE相比,P = 0.078)。对于大多数SLE患者,未观察到总体库多样性与临床疾病活动之间存在显著相关性,11例SLE患者中只有2例在病情发作时间点附近库多样性呈下降趋势。我们未观察到所有SLE患者中前100个扩增克隆之间CDR3氨基酸序列的任何重叠或Vβ或Jβ基因的优先使用情况。在HC和SLE中,大多数扩增克隆随时间推移都非常稳定(HC = 5.5±0.5个月,SLE = 7.2±2.4个月)。
结论
与HC相比,SLE患者的PB中观察到T细胞库多样性显著降低。然而,在大多数SLE患者中,随着疾病活动增加至病情发作,库多样性并未显著变化。因此,在没有疾病特异性克隆的先验知识的情况下,监测SLE患者PB中的TCR库不太可能用于预测疾病活动的变化。
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