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通过光谱分型鉴定无功能肾移植中扩增的T细胞克隆。

Identification of expanded T-cell clones by spectratyping in nonfunctioning kidney transplants.

作者信息

Cappuccilli Maria, Donati Gabriele, Comai Giorgia, Baraldi Olga, Conte Diletta, Capelli Irene, Aiello Valeria, Pession Andrea, La Manna Gaetano

机构信息

Department of Experimental Diagnostic and Specialty Medicine (DIMES), Nephrology, Dialysis, and Renal Transplant Unit.

Molecular Laboratory of Pediatrics, Hematology-Oncology Unit, St Orsola Hospital, University of Bologna, Bologna, Italy.

出版信息

J Inflamm Res. 2017 May 3;10:41-47. doi: 10.2147/JIR.S124944. eCollection 2017.

Abstract

BACKGROUND

The aim of this study was the application of complementarity-determining region-3 spectratyping analysis to determine T-cell-repertoire complexity and to detect T-cell-clone expansion, as a measure of immune response in nonfunctioning kidney transplants (group hemodialysis-transplant [HD-Tx]), nontransplanted dialysis patients (group hemodialysis [HD]), and normal subjects as controls (group C).

PATIENTS AND METHODS

Analysis of T-cell receptor (TCR) diversity by spectratyping was applied to peripheral blood samples collected from 21 subjects: eight in group HD-Tx, seven in group HD, and six in group C.

RESULTS

Considering the extent of the skew in TCR variable region repertoires as a measure of clonal T cells, we found that the number of altered spectra showed a progressive increase from normal subjects to dialysis patients and to nonfunctioning kidney transplants, respectively. Healthy subjects had the lowest number of altered spectra, and patients with nonfunctioning kidney transplants the highest. Differences were significant for group HD-Tx vs group C (=0.017) and group HD vs group C (=0.015), but not between nonfunctioning kidney-transplant recipients and dialysis patients (group HD-Tx vs group HD).

CONCLUSION

Although dialysis appears to be a weaker trigger for clonal expansion of T cells, our data suggest that the utilization of complementarity-determining region-3 spectratyping analysis of the TCR repertoire might be useful to monitor specific immunoactivation in patients before and after kidney transplantation.

摘要

背景

本研究的目的是应用互补决定区-3 谱型分析来确定 T 细胞库的复杂性并检测 T 细胞克隆扩增,以此作为无功能肾移植患者(血液透析-移植组[HD-Tx])、未接受移植的透析患者(血液透析组[HD])以及作为对照的正常受试者(C 组)免疫反应的一项指标。

患者与方法

采用谱型分析对 21 名受试者采集的外周血样本进行 T 细胞受体(TCR)多样性分析,其中 HD-Tx 组 8 例,HD 组 7 例,C 组 6 例。

结果

将 TCR 可变区库的偏斜程度作为克隆性 T 细胞的一项指标,我们发现改变的谱型数量分别从正常受试者到透析患者再到无功能肾移植患者呈逐渐增加趋势。健康受试者改变的谱型数量最少,无功能肾移植患者最多。HD-Tx 组与 C 组(P = 0.017)以及 HD 组与 C 组(P = 0.015)之间差异有统计学意义,但无功能肾移植受者与透析患者之间(HD-Tx 组与 HD 组)无差异。

结论

尽管透析似乎是 T 细胞克隆扩增较弱的触发因素,但我们的数据表明,利用 TCR 库的互补决定区-3 谱型分析可能有助于监测肾移植患者术前和术后的特异性免疫激活情况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5de/5422501/ffa9211d058e/jir-10-041Fig1.jpg

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