Lymph node and circulating T cell characteristics are strongly correlated in end‐stage renal disease patients, but highly differentiated T cells reside within the circulation

B. Dedeoglu, A. D. Weerd, Ling Huang, A. Langerak, Frank J. M. F. Dor, M. Klepper, W. Verschoor, Derek Reijerkerk, C. Baan, N. H. Litjens, M. Betjes
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引用次数: 14

Abstract

Ageing is associated with changes in the peripheral T cell immune system, which can be influenced significantly by latent cytomegalovirus (CMV) infection. To what extent changes in circulating T cell populations correlate with T cell composition of the lymph node (LN) is unclear, but is crucial for a comprehensive understanding of the T cell system. T cells from peripheral blood (PB) and LN of end‐stage renal disease patients were analysed for frequency of recent thymic emigrants using CD31 expression and T cell receptor excision circle content, relative telomere length and expression of differentiation markers. Compared with PB, LN contained relatively more CD4+ than CD8+ T cells (P < 0·001). The percentage of naive and central memory CD4+ and CD8+ T cells and thymic output parameters showed a strong linear correlation between PB and LN. Highly differentiated CD28null T cells, being CD27–, CD57+ or programmed death 1 (PD‐1+), were found almost exclusively in the circulation but not in LN. An age‐related decline in naive CD4+ and CD8+ T cell frequency was observed (P = 0·035 and P = 0·002, respectively) within LN, concomitant with an increase in central memory CD8+ T cells (P = 0·033). Latent CMV infection increased dramatically the frequency of circulating terminally differentiated T cells, but did not alter T cell composition and ageing parameters of LN significantly. Overall T cell composition and measures of thymic function in PB and LN are correlated strongly. However, highly differentiated CD28null T cells, which may comprise a large part of circulating T cells in CMV‐seropositive individuals, are found almost exclusively within the circulation.
在终末期肾病患者中,淋巴结和循环T细胞特征密切相关,但高度分化的T细胞存在于循环中
衰老与外周T细胞免疫系统的变化有关,这可能受到潜伏巨细胞病毒(CMV)感染的显著影响。循环T细胞群的变化在多大程度上与淋巴结(LN)的T细胞组成相关尚不清楚,但这对于全面了解T细胞系统至关重要。采用CD31表达、T细胞受体切除环含量、相对端粒长度和分化标志物表达等方法,分析终末期肾病患者外周血(PB)和LN中的T细胞近期胸腺移行频率。与PB相比,LN细胞CD4+含量明显高于CD8+ T细胞(P < 0.001)。原始记忆和中枢记忆CD4+和CD8+ T细胞百分比和胸腺输出参数在PB和LN之间显示出很强的线性相关性。高度分化的CD28null T细胞,即CD27 -、CD57+或程序性死亡1 (PD‐1+),几乎全部存在于循环中,而不存在于LN中。在LN中观察到与年龄相关的初始CD4+和CD8+ T细胞频率下降(P分别= 0.035和0.002),同时伴有中央记忆CD8+ T细胞增加(P = 0.033)。潜伏CMV感染显著增加循环终末分化T细胞的频率,但未显著改变LN的T细胞组成和老化参数。总体T细胞组成和胸腺功能测量在PB和LN中有很强的相关性。然而,高度分化的CD28null T细胞,可能在CMV血清阳性个体的循环T细胞中占很大一部分,几乎只在循环中发现。
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