大规模血清蛋白质组学鉴定与杜兴氏肌肉萎缩症患者表现下降和临床里程碑相关的蛋白质

Nadine Ikelaar, Alison Barnard, Simon Eng, Sharzad Hosseini Vajargah, Kevin Ha, Hermien Kan, Krista Vandenborne, Erik Niks, Glenn Walter, Pietro Spitali
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引用次数: 0

摘要

在杜氏肌营养不良症(DMD)的临床研究中,血清生物标志物是很有前途的微创结果测量指标。然而,目前还缺乏与临床进展密切相关并能预测机能下降的生物标志物。在本研究中,我们旨在确定与临床表现相关并能预测 DMD 临床里程碑的血清生物标志物。为此,我们开展了一项回顾性多中心队列研究,其中包括作为佛罗里达大学(UF)自然史研究一部分的 DMD 研究参与者的血清样本和临床数据,以及 2009-2022 年间莱顿大学医学中心(LUMC)的实际观察结果。7K SomaScan 分析法用于分析个体血清样本中的蛋白质水平。血清生物标志物可预测丧失行动能力(LoA)的年龄、丧失高空伸展能力(OHR)的年龄和丧失手到口功能(HTM)的年龄。次要结果是生物标志物与年龄、皮质类固醇(CS)使用情况和临床表现(基于北极星非卧床评估(NSAA)、10 米跑速度(10mrv)、6 分钟步行(6MWT)和上肢表现(PUL2.0))的关系。研究人员共采集了 716 份血清样本,其中和睦家医院 79 人,路睦家医院 74 人(平均[标码]年龄;10.9[3.2] 对 8.4[3.4])。244个血清蛋白显示,在两个组群中,CS的使用与CS类型和治疗方案无关,其中包括MMP3和IGLL1。在两个队列中,318个探针(对应294个蛋白质)与NSAA、10mrv、6MWT和/或PUL2.0有显著相关性。在 LUMC 和 UF 队列中,38 个探针(对应 36 种蛋白质,如 RGMA、EHMT2、ART3、ANTXR2 和 DLK1)的表达与下肢和上肢临床里程碑的风险相关。总之,多种生物标志物与 DMD 患者使用 CS、运动功能和上下肢疾病里程碑相关。这些生物标志物在两个独立的队列中得到了验证,从而提高了它们在更广泛的 DMD 群体中应用的可能性。
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Large scale serum proteomics identifies proteins associated with performance decline and clinical milestones in Duchenne muscular dystrophy
Serum biomarkers are promising minimally invasive outcome measures in clinical studies in Duchenne muscular dystrophy (DMD). However, biomarkers strongly associated with clinical progression and predicting performance decline are lacking. In this study we aimed to identify serum biomarkers associated with clinical performance and able to predict clinical milestones in DMD. Towards this aim we present a retrospective multi-center cohort study including serum samples and clinical data collected in research participants with DMD as part of a natural history study at the University of Florida (UF) and real-world observations at Leiden University Medical Center (LUMC) between 2009-2022. The 7K SomaScan assay was used to analyse protein levels in in individual serum samples. Serum biomarkers predicted age at loss of ambulation (LoA), age at loss of overhead reach (OHR) and age at loss of hand to mouth function (HTM). Secondary outcomes were the association of biomarkers with age, corticosteroid (CS) usage, and clinical performance based on the North Star Ambulatory Assessment (NSAA), 10 meter run velocity (10mrv), 6 minute walk (6MWT) and Performance of the Upper Limb (PUL2.0). A total of 716 serum samples were collected in 79 participants at UF and 74 at LUMC (mean[SD] age; 10.9[3.2] vs 8.4[3.4]). 244 serum proteins showed an association with CS usage in both cohorts independent of CS type and regimen, including MMP3 and IGLL1. 318 probes (corresponding to 294 proteins) showed significant associations with NSAA, 10mrv, 6MWT and/or PUL2.0 across both cohorts. The expression of 38 probes corresponding to 36 proteins such as RGMA, EHMT2, ART3, ANTXR2 and DLK1 was associated with risk of both lower and upper limb clinical milestones in both the LUMC and UF cohort. In conclusion, multiple biomarkers were associated with CS use, motor function and upper lower and upper limb disease milestones in DMD. These biomarkers were validated across two independent cohorts, increasing their likelihood of translation for use within the broader DMD population.
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