Identification and evolution of predictors of Sjögren's disease-associated mucosa-associated lymphoid tissue lymphoma development over time: a case-control study

IF 15 1区 医学 Q1 RHEUMATOLOGY Lancet Rheumatology Pub Date : 2024-08-22 DOI:10.1016/S2665-9913(24)00183-8
Andreas V Goules PhD , Loukas Chatzis PhD , Vasilis C Pezoulas PhD , Markos Patsouras PhD , Prof Clio Mavragani PhD , Prof Luca Quartuccio PhD , Prof Chiara Baldini PhD , Prof Salvatore De Vita PhD , Prof Dimitrios I Fotiadis PhD , Prof Athanasios G Tzioufas PhD
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引用次数: 0

Abstract

Background

Non-Hodgkin lymphomas have a substantial impact on individuals with Sjögren's disease. This study focuses on mucosal-associated lymphoid tissue (MALT) lymphomas, which constitute the majority of Sjögren's disease-associated non-Hodgkin lymphomas. We aimed to identify reliable lymphoma predictors in patients with Sjögren's disease and study their progression over time.

Methods

In this case-control study, patients diagnosed with Sjögren's disease-associated MALT lymphoma, with a minimum of 3 years between Sjögren's disease diagnosis and MALT lymphoma diagnosis, were included from three centres specialising in Sjögren's disease (University of Athens, Athens, Greece; University of Pisa, Pisa, Italy; and University of Udine, Udine, Italy) and matched 1:1 with control participants with Sjögren's disease who did not have lymphoma according to age, sex, disease duration at last follow up, and treatment modality. Three harmonised datasets were constructed, curated, and analysed to identify MALT lymphoma predictors, representing three distinct timepoints in lymphomagenesis progression: V1 at Sjögren's disease diagnosis, V2 3–4 years before lymphoma diagnosis, and V3 0·5–1·5 years before lymphoma diagnosis. All recruited patients fulfilled the 2016 American College of Rheumatology–European League Against Rheumatism criteria for Sjögren's disease. The primary outcome was to identify MALT lymphoma predictors in Sjögren's disease, present at the timepoint of Sjögren's disease diagnosis and 3–4 years before the diagnosis of MALT lymphoma. A fast correlation-based feature selection and logistic regression model was used at V1 and V2 to identify MALT lymphoma predictors. The progression of potential predictors was studied across V1, V2, and V3. Histological parameters were not included in the analysis. An individual with lived experience of Sjögren's disease was involved in the study design.

Findings

80 patients with Sjögren's disease-associated MALT lymphoma were included in the V1 dataset, 68 in the V2 dataset, and 80 in the V3 dataset, and matched to control participants with Sjögren's disease who did not have lymphoma. In both groups, 72 (90%) of 80 participants were women and eight (10%) were men. The mean age at Sjögren's disease diagnosis was 48·6 years (SD 11·6) in the lymphoma group and 48·7 years (11·5) in the control group. All patients were White, with 88 (55%) of 160 individuals of Greek nationality and 72 (45%) of Italian nationality. At the V1 timepoint, rheumatoid factor was the only independent lymphoma predictor (odds ratio 3·33 [95% CI 1·96–5·64]). At the V2 timepoint, rheumatoid factor (3·66 [95% CI 2·08–6·42]) and European League Against Rheumatism Sjögren's Syndrome Disease Activity Index ≥5 (3·88 [1·69–8·90]) were identified as independent lymphoma risk factors. The high disease activity during the transition from the V1 to V2 timepoint was attributed to specific B-cell-derived manifestations, including cryoglobulinaemia and glandular, cutaneous, and hematological manifestations.

Interpretation

Following up patients with high-risk of Sjögren's disease-associated MALT lymphoma based on the temporal progression of predictors presents an opportunity for early diagnosis and potential therapeutic interventions. Rheumatoid factor was the earliest and most persistent independent predictor of lymphoma. Specific B-cell manifestations in combination with rheumatoid factor indicate a more advanced stage of the lymphomagenesis process.

Funding

European Commission—Horizon 2020.
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病例对照研究:识别和演化斯约戈伦氏病相关粘膜相关淋巴组织淋巴瘤随时间发展的预测因素。
背景:非霍奇金淋巴瘤对患有斯约戈伦病的患者有很大影响。本研究的重点是粘膜相关淋巴组织(MALT)淋巴瘤,这种淋巴瘤在与斯约金病相关的非霍奇金淋巴瘤中占大多数。我们的目的是在斯约格伦病患者中找出可靠的淋巴瘤预测指标,并研究它们随时间的进展情况:在这项病例对照研究中,我们纳入了三所专治斯约戈伦病的中心(希腊雅典的雅典大学、意大利比萨的比萨大学和意大利乌迪内的乌迪内大学)诊断出的斯约戈伦病相关 MALT 淋巴瘤患者,这些患者的斯约戈伦病诊断与 MALT 淋巴瘤诊断之间至少相隔 3 年:根据年龄、性别、最后一次随访时的病程和治疗方式,与未患淋巴瘤的斯约格伦病对照组患者进行1:1配对。我们构建、整理和分析了三个统一的数据集,以确定 MALT 淋巴瘤的预测因子,这三个数据集代表了淋巴瘤发生发展过程中三个不同的时间点:V1 在确诊 Sjögren's 病时,V2 在淋巴瘤确诊前 3-4 年,V3 在淋巴瘤确诊前 0-5-1-5 年。所有招募的患者均符合2016年美国风湿病学会-欧洲抗风湿联盟的斯约格伦病标准。主要研究结果是确定斯约戈伦病的MALT淋巴瘤预测因子,这些因子存在于斯约戈伦病诊断的时间点和MALT淋巴瘤诊断前3-4年。在 V1 和 V2 处使用了基于快速相关性的特征选择和逻辑回归模型来识别 MALT 淋巴瘤预测因子。研究了潜在预测因子在 V1、V2 和 V3 中的进展情况。组织学参数未纳入分析。一名具有斯约恩氏病生活经验的人士参与了研究设计:V1数据集包括80名与斯约格伦病相关的MALT淋巴瘤患者,V2数据集包括68名患者,V3数据集包括80名患者,并与未患淋巴瘤的斯约格伦病对照参与者进行了配对。在这两组 80 名参与者中,72 人(90%)为女性,8 人(10%)为男性。淋巴瘤组患者确诊为斯约格伦病时的平均年龄为 48-6 岁(标准差 11-6),对照组为 48-7 岁(标准差 11-5)。所有患者均为白人,160 人中有 88 人(55%)为希腊人,72 人(45%)为意大利人。在 V1 时间点,类风湿因子是唯一独立的淋巴瘤预测因子(几率比 3-33 [95% CI 1-96-5-64])。在 V2 时间点,类风湿因子(3-66 [95% CI 2-08-6-42])和欧洲抗风湿病联盟 Sjögren's 综合征疾病活动指数≥5(3-88 [1-69-8-90])被确定为独立的淋巴瘤风险因素。从 V1 到 V2 时间点过渡期间的高疾病活动性归因于特定的 B 细胞衍生表现,包括低温球蛋白血症以及腺体、皮肤和血液学表现:解读:根据预测因子的时间进展情况,对与斯约格伦病相关的MALT淋巴瘤高危患者进行随访,为早期诊断和潜在的治疗干预提供了机会。类风湿因子是最早也是最持久的淋巴瘤独立预测因子。特异性B细胞表现与类风湿因子相结合,表明淋巴瘤发病过程已进入晚期:资助:欧盟委员会-地平线2020。
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来源期刊
Lancet Rheumatology
Lancet Rheumatology RHEUMATOLOGY-
CiteScore
34.70
自引率
3.10%
发文量
279
期刊介绍: The Lancet Rheumatology, an independent journal, is dedicated to publishing content relevant to rheumatology specialists worldwide. It focuses on studies that advance clinical practice, challenge existing norms, and advocate for changes in health policy. The journal covers clinical research, particularly clinical trials, expert reviews, and thought-provoking commentary on the diagnosis, classification, management, and prevention of rheumatic diseases, including arthritis, musculoskeletal disorders, connective tissue diseases, and immune system disorders. Additionally, it publishes high-quality translational studies supported by robust clinical data, prioritizing those that identify potential new therapeutic targets, advance precision medicine efforts, or directly contribute to future clinical trials. With its strong clinical orientation, The Lancet Rheumatology serves as an independent voice for the rheumatology community, advocating strongly for the enhancement of patients' lives affected by rheumatic diseases worldwide.
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