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两个临床队列中造血干细胞移植后全CDR3 T细胞受体库分析

Analysis of the Whole CDR3 T Cell Receptor Repertoire after Hematopoietic Stem Cell Transplantation in 2 Clinical Cohorts.

作者信息

Shah Omid, Tamaresis John S, Kenyon Laura Jean, Xu Liwen, Zheng Pingping, Gupta Puja, Rangarajan Krish, Lee Stephanie, Spellman Stephen, Nikiforow Sarah, Zehnder James, Meyer Everett H

机构信息

Division of Blood and Marrow Transplantation, Stanford University School of Medicine, Stanford, California.

Department of Biomedical Data Science, Stanford University School of Medicine, Stanford, California.

出版信息

Biol Blood Marrow Transplant. 2020 Jun;26(6):1050-1070. doi: 10.1016/j.bbmt.2020.01.020. Epub 2020 Feb 18.

Abstract

A major cause of morbidity and mortality for patients who undergo hematologic stem cell transplantation (HSCT) is acute graft-versus-host disease (aGVHD), a mostly T cell-mediated disease. Examination of the T cell receptor (TCR) repertoire of HSCT recipients and the use of next-generation nucleotide sequencing have raised the question of whether features of TCR repertoire reconstitution might reproducibly associate with aGVHD. We hypothesized that the peripheral blood TCR repertoire of patients with steroid-nonresponsive aGVHD would be less diverse. We also hypothesized that patients with GVHD who shared HLA might also share common clones at the time of GVHD diagnosis, thereby potentially providing potential clinical indicators for treatment stratification. We further hypothesized that HSCT recipients with the same HLA mismatch might share a more similar TCR repertoire based on a potentially shared focus of alloreactive responses. We studied 2 separate patient cohorts and 2 separate platforms for measuring TCR repertoire. The first cohort of patients was from a multicenter Phase III randomized double-blinded clinical trial of patients who developed aGVHD (NCT01002742). The second cohort comprised samples from biobanks from 2 transplantation centers and the Center for International Blood and Marrow Transplant Research of patients who underwent mismatched HSCT. There were no statistically significant differences in the TCR diversity of steroid responders and nonresponders among patients with aGVHD on the day of diagnosis. Most clones in the repertoire were unique to each patient, but a small number of clones were found to be both exclusive to and shared among aGVHD nonresponders. We were also able to show a strong correlation between the presence of Vβ20 and Vβ29 and steroid responsiveness. Using the Bhattacharya coefficient, those patients who shared the same HLA mismatch were shown to be no more similar to one another than to those who had a completely different mismatch. Using 2 separate clinical cohorts and 2 separate platforms for analyzing the TCR repertoire, we have shown that the sampled human TCR repertoire is largely unique to each patient but contains glimmers of common clones of subsets of clones based on responsiveness to steroids in aGVHD on the day of diagnosis. These studies are informative for future strategies to assess for reproducible TCR responses in human alloreactivity and possible markers of GVHD responsiveness to therapy.

摘要

接受血液学干细胞移植(HSCT)患者发病和死亡的一个主要原因是急性移植物抗宿主病(aGVHD),这是一种主要由T细胞介导的疾病。对HSCT受者的T细胞受体(TCR)库进行检测以及使用下一代核苷酸测序引发了这样一个问题,即TCR库重建的特征是否可能与aGVHD存在可重复性关联。我们假设,对类固醇无反应的aGVHD患者的外周血TCR库多样性较低。我们还假设,患有移植物抗宿主病且HLA相同的患者在移植物抗宿主病诊断时也可能共享共同的克隆,从而有可能为治疗分层提供潜在的临床指标。我们进一步假设,具有相同HLA错配的HSCT受者可能基于潜在的共同同种异体反应焦点而共享更相似的TCR库。我们研究了2个独立的患者队列以及2个用于测量TCR库的独立平台。第一组患者来自一项针对发生aGVHD患者的多中心III期随机双盲临床试验(NCT01002742)。第二组包括来自2个移植中心生物样本库以及国际血液和骨髓移植研究中心的接受错配HSCT患者的样本。在诊断当天,aGVHD患者中类固醇反应者和无反应者的TCR多样性在统计学上无显著差异。库中的大多数克隆对每个患者而言都是独特的,但发现少数克隆是aGVHD无反应者所特有的且在他们之间共享。我们还能够证明Vβ20和Vβ29的存在与类固醇反应性之间存在很强的相关性。使用巴塔查里亚系数,结果显示具有相同HLA错配的患者之间并不比那些具有完全不同错配的患者彼此更相似。通过使用2个独立的临床队列和2个独立的平台来分析TCR库,我们已经表明,所采样的人类TCR库在很大程度上对每个患者而言都是独特的,但在诊断当天的aGVHD中,基于对类固醇的反应性,包含了克隆亚群共同克隆的些许迹象。这些研究对于未来评估人类同种异体反应中可重复性TCR反应以及移植物抗宿主病治疗反应可能标志物的策略具有参考价值。

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