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Ribosomal and Immune Transcripts Associate with Relapse in Acquired ADAMTS13-Deficient Thrombotic Thrombocytopenic Purpura.

机译:核糖体和免疫转录物与获得性ADAMTS13缺陷型血栓性血小板减少性紫癜的复发相关。

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摘要

Approximately 40% of patients who survive acute episodes of thrombotic thrombocytopenic purpura (TTP) associated with severe acquired ADAMTS13 deficiency experience one or more relapses. Risk factors for relapse other than severe ADAMTS13 deficiency and ADAMTS13 autoantibodies are unknown. ADAMTS13 autoantibodies, TTP episodes following infection or type I interferon treatment and reported ensuing systemic lupus erythematosus in some patients suggest immune dysregulation. This cross-sectional study asked whether autoantibodies against RNA-binding proteins or peripheral blood gene expression profiles measured during remission are associated with history of prior relapse in acquired ADAMTS13-deficient TTP. Peripheral blood from 38 well-characterized patients with autoimmune ADAMTS13-deficient TTP in remission was examined for autoantibodies and global gene expression. A subset of TTP patients (9 patients, 24%) exhibited a peripheral blood gene signature composed of elevated ribosomal transcripts that associated with prior relapse. A non-overlapping subset of TTP patients (9 patients, 24%) displayed a peripheral blood type I interferon gene signature that associated with autoantibodies to RNA-binding proteins but not with history of relapse. Patients who had relapsed bimodally expressed higher HLA transcript levels independently of ribosomal transcripts. Presence of any one potential risk factor (ribosomal gene signature, elevated HLA-DRB1, elevated HLA-DRB5) associated with relapse (OR = 38.4; p = 0.0002) more closely than any factor alone or all factors together. Levels of immune transcripts typical of natural killer (NK) and T lymphocytes positively correlated with ribosomal gene expression and number of prior episodes but not with time since the most recent episode. Flow cytometry confirmed elevated expression of cell surface markers encoded by these transcripts on T and/or NK cell subsets of patients who had relapsed. These data associate elevated ribosomal and immune transcripts with relapse history in acquired, ADAMTS13-deficient TTP.
机译:幸存下来的与严重后天性ADAMTS13缺乏症相关的血栓性血小板减少性紫癜(TTP)急性发作的患者中约有40%经历了一次或多次复发。除了严重的ADAMTS13缺乏症和ADAMTS13自身抗体以外,复发的危险因素尚不清楚。 ADAMTS13自身抗体,感染或I型干扰素治疗后的TTP发作以及据报道,随后在某些患者中出现系统性红斑狼疮提示免疫功能异常。这项横断面研究询问缓解期间测量的针对RNA结合蛋白的自身抗体或外周血基因表达谱是否与获得性ADAMTS13缺陷型TTP的先前复发史相关。检查了38例特征明确的自身免疫性ADAMTS13缺陷型TTP缓解患者的外周血自身抗体和整体基因表达。一部分TTP患者(9名患者,24%)显示出外周血基因特征,该特征由与先前复发相关的核糖体转录本升高构成。 TTP患者的一个非重叠子集(9名患者,24%)显示出外周血I型干扰素基因标志,该标志物与针对RNA结合蛋白的自身抗体有关,但与复发史无关。复发的双峰患者独立于核糖体转录本表达较高的HLA转录水平。与复发相关的任何一种潜在危险因素(核糖体基因特征,HLA-DRB1升高,HLA-DRB5升高)的存在(OR = 38.4; p = 0.0002)比任何单独的因素或所有因素加在一起更为紧密。自然杀手(NK)和T淋巴细胞的典型免疫转录水平与核糖体基因表达和先前发作次数呈正相关,但与最近一次发作后的时间无关。流式细胞术证实了这些转录本编码的细胞表面标志物在复发患者的T和/或NK细胞亚群中表达升高。这些数据将核糖体和免疫转录物的升高与获得性ADAMTS13缺陷型TTP的复发史联系起来。

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