预测意义未定的克隆性细胞减少症患者的细胞减少症、病情进展和存活率:一项前瞻性队列研究

Catherine Cargo, Elsa Bernard, Tumas Beinortas, Kelly L Bolton, Paul Glover, Helen Warren, Daniel Payne, Rukhsaar Ali, Alesia Khan, Mike Short, Suzan Van Hoppe, Alex Smith, Jan Taylor, Paul Evans, Elli Papaemmanuil, Simon Crouch
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引用次数: 0

摘要

背景据报道,在患有细胞减少症但未确诊为血液病的患者中,经常会出现基因突变(意义未定的克隆性细胞减少症;CCUS)。与没有此类突变的患者相比,这些患者进展为髓系恶性肿瘤的风险更高,总生存率更低。迄今为止,由于回顾性分析或患者人数较少,研究受到了限制。我们的目的是通过前瞻性地调查一个庞大、定义明确的患者队列的结果来确定CCUS的自然史。方法这项前瞻性队列研究在英国利兹的一个诊断实验室--血液恶性肿瘤诊断服务处进行。年龄在 18 岁以上、转诊接受细胞减少症检查的患者均符合纳入条件;有髓系恶性肿瘤病史的患者不符合纳入条件。在进行常规临床检测的同时还进行了靶向测序。基线突变分析与主要研究结果相关联:纵向血细胞计数、髓系恶性肿瘤疾病进展和中位随访 4-54 年(IQR 4-03-5-04)的总生存期。数据由人工从医院记录中收集,或从实验室或临床结果数据库中提取。研究结果血液恶性肿瘤诊断服务机构在2014年7月1日至2016年7月31日期间接收了2348名患者的骨髓样本。其中2083名患者(中位年龄72岁[IQR 63-80,范围18-99];854名[41-0%]女性和1229名[59-0%]男性)符合纳入标准,且样本质量足以进行进一步分析。598例(28-7%)患者根据活检样本获得诊断,1485例(71-3%)样本被归类为非诊断样本;其中,400例(26-9%)患者(256例[64-0%]男性和144例[36-0%]女性)确诊为CCUS。TET2、SRSF2和DNMT3A是CCUS患者中最常发生突变的基因,400名患者中有320人(80%)至少有一个基因发生了突变。年龄(p<0-0001)、性别(p=0-0027)以及ASXL1(p=0-0009)、BCOR(p=0-0056)和TP53(p=0-0055)的突变与总生存率的降低有关;然而,突变的数量是预测进展为髓系恶性肿瘤的最强因素(两个突变,p=0-0024;三个或更多突变,p=0-0004)。对具有连续样本且初始髓系基因面板中无突变的亚组患者样本进行扩展测序后发现,DDX41 和 UBA1 均存在复发性突变,这表明临床检测面板中应包括这些基因。高风险基因突变和突变数量的增加可预测发病后 5 年内的存活率和病情进展,因此需要进行临床监测,并在必要时采取干预措施。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Predicting cytopenias, progression, and survival in patients with clonal cytopenia of undetermined significance: a prospective cohort study

Background

Somatic mutations are frequently reported in individuals with cytopenia but without a confirmed haematological diagnosis (clonal cytopenia of undetermined significance; CCUS). These patients have an increased risk of progression to a myeloid malignancy and worse overall survival than those with no such mutations. To date, studies have been limited by retrospective analysis or small patient numbers. We aimed to establish the natural history of CCUS by prospectively investigating outcome in a large, well defined patient cohort.

Methods

This prospective cohort study was conducted at the Haematological Malignancy Diagnostic Service, a diagnostic laboratory in Leeds, UK. Patients aged at least 18 years who were referred for investigation of cytopenia were eligible for inclusion; those with a history of myeloid malignancy were not eligible. Targeted sequencing was conducted alongside routine clinical testing. Baseline mutation analysis was then correlated with the main study outcomes: longitudinal blood counts, disease progression to a myeloid malignancy, and overall survival with a median follow-up of 4·54 years (IQR 4·03–5·04). Data were collected manually from hospital records or extracted from laboratory or clinical outcome databases.

Findings

Bone marrow samples from 2348 patients were received at the Haematological Malignancy Diagnostic Service between July 1, 2014, and July 31, 2016. Of these, 2083 patients (median age 72 years [IQR 63–80, range 18–99]; 854 [41·0%] female and 1229 [59·0%] male) met the inclusion criteria and had samples of sufficient quality for further analysis. 598 (28·7%) patients received a diagnosis on the basis of their biopsy sample, whereas 1485 (71·3%) samples were classified as non-diagnostic; of these, CCUS was confirmed in 400 (26·9%) patients (256 [64·0%] male and 144 [36·0%] female). TET2, SRSF2, and DNMT3A were the most frequently mutated genes in patients with CCUS, with 320 (80%) of 400 patients harbouring a mutation in at least one of these genes. Age (p<0·0001), sex (p=0·0027), and mutations in ASXL1 (p=0·0009), BCOR (p=0·0056), and TP53 (p=0·0055) correlated with a worse overall survival; however, the number of mutations was the strongest predictor for progression to a myeloid malignancy (two mutations, p=0·0024; three or more mutations, p=0·0004). Extended sequencing of samples from a subgroup of patients with sequential samples and no mutations in the initial myeloid gene panel showed recurrent mutations in both DDX41 and UBA1, suggesting that these genes should be included in clinical test panels.

Interpretation

Mutation analysis is advised in patients who have undergone bone marrow examination and have an otherwise-unexplained cytopenia. High-risk genetic mutations and increased numbers of mutations are predictive of both survival and progression within 5 years of presentation, warranting clinical surveillance and, when necessary, intervention.

Funding

MDS Foundation.

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