先天性免疫错误是大颗粒淋巴细胞白血病克隆T细胞扩增的基础。

The Journal of Clinical Investigation Pub Date : 2025-05-01 DOI:10.1172/jci184431

Carlos Bravo-Perez,Carmelo Gurnari,Jani Huuhtanen,Naomi Kawashima,Luca Guarnera,Aashray Mandala,Nakisha D Williams,Christopher Haddad,Michaela Witt,Serhan Unlu,Zachary Brady,Olisaemeka Ogbue,Mark Orland,Arooj Ahmed,Yasuo Kubota,Simona Pagliuca,Arda Durmaz,Satu Mustjoki,Valeria Visconte,Jaroslaw P Maciejewski

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引用次数: 0

摘要

背景：T细胞大颗粒淋巴细胞白血病（T- lgll）是一种细胞毒性T淋巴细胞（ctl）的淋巴增生性疾病，通常伴有功能获得性STAT3突变。T-LGLL是研究持续性CTL扩增的独特模型。尽管自身免疫是隐含的，但各种矛盾的观察结果使我们调查免疫缺陷特征是否支持T-LGLL。方法：这是一项全面的免疫基因组研究，来自一个具有完整实验室-临床特征的大型T-LGLL队列的92例连续患者（n = 271）。分析了T细胞淋巴驱动因子中与先天性免疫错误（IEI）和体细胞突变相关的变异的全外显子组谱。利用T- lgll样本中的单细胞RNA-Seq和TCR-Seq以及T细胞癌细胞系中的RNA-Seq来建立生物学相关性。结果241例T-LGLL患者中有186例（77%）存在淋巴细胞减少症和/或低丙种球蛋白血症。IEI遗传筛查显示，92例患者中34例（36%）在38种不同的免疫基因中发现43种罕见的杂合变异（对照组为167/63,026[0.26%]）。92例患者中有15例（16%）检测到与显性成人发病iei相关的高置信度有害变异。携带者表现出与隐匿性IEI相关的非典型特征，如发病较早，淋巴细胞计数较低，STAT3突变率较低，低γ -球蛋白血症和免疫细胞减少/骨髓衰竭的比例高于非携带者。体细胞突变景观、RNA-Seq和TCR-Seq分析支持由IEI变异和与T细胞淋巴细胞驱动体突变的相互作用引起的免疫失衡。结论在T-LGLL中的研究结果表明，不适应的CTL扩增可能源于隐性免疫缺陷特征，这为iei向克隆造血和骨髓衰竭的发展打开了视野。再生障碍性贫血和MDS国际基金会；VeloSano;爱德华·埃文斯基金会；卡洛斯三世研究所；欧洲研究理事会；欧洲个体化医疗研究区域网；学院芬兰;芬兰癌症基金会。

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Inborn errors of immunity underlie clonal T cell expansions in large granular lymphocyte leukemia.

BACKGROUNDT cell large granular lymphocyte leukemia (T-LGLL) is a lymphoproliferative disorder of cytotoxic T lymphocytes (CTLs), often with gain-of-function STAT3 mutations. T-LGLL represents a unique model for the study of persistent CTL expansions. Albeit autoimmunity is implied, various paradoxical observations led us to investigate whether immunodeficiency traits underpin T-LGLL.METHODSThis is a comprehensive immunogenomic study of 92 consecutive patients from a large T-LGLL cohort with full laboratory-clinical characterization (n = 271). Whole-exome profiling of variants associated with inborn errors of immunity (IEI) and somatic mutations in T cell lymphoid drivers was analyzed. Single-cell RNA-Seq and TCR-Seq in T-LGLL samples and RNA-Seq in T cell cancer cell lines were utilized to establish biological correlations.RESULTSLymphocytopenia and/or hypogammaglobulinemia were identified in 186 of 241 (77%) T-LGLL patients. Genetic screening for IEI revealed 43 rare heterozygous variants in 38 different immune genes in 34 of 92 (36%) patients (vs. 167/63,026 [0.26%] in controls). High-confidence deleterious variants associated with dominant, adult-onset IEIs were detected in 15 of 92 (16%) patients. Carriers showed atypical features otherwise tied to the cryptic IEI, such as earlier onset, lower lymphocyte counts, lower STAT3 mutational rate, and higher proportions of hypogammaglobulinemia and immune cytopenia/bone marrow failure than noncarriers. Somatic mutational landscape, RNA-Seq, and TCR-Seq analyses supported immune imbalance caused by the IEI variants and interactions with somatic mutations in T cell lymphoid drivers.CONCLUSIONSOur findings in T-LGLL reveal that maladaptive CTL expansions may stem from cryptic immunodeficiency traits and open the horizon of IEIs to clonal hematopoiesis and bone marrow failure.FUNDINGNIH; Aplastic Anemia and MDS International Foundation; VeloSano; Edward P. Evans Foundation; Instituto de Salud Carlos III; European Research Council; European Research Area Network on Personalised Medicine; Academy Finland; Cancer Foundation Finland.

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The Journal of Clinical Investigation

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