血浆 ALS 和 Gal-3BP 可区分 MASLD 患者的早期和晚期肝纤维化

IF 9.5 2区 医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL Biomarker Research Pub Date : 2024-04-29 DOI:10.1186/s40364-024-00583-z
David Pérez Compte, Lucas Etourneau, Anne-Marie Hesse, Alexandra Kraut, Justine Barthelon, Nathalie Sturm, Hélène Borges, Salomé Biennier, Marie Courçon, Marc de Saint Loup, Victoria Mignot, Charlotte Costentin, Thomas Burger, Yohann Couté, Christophe Bruley, Thomas Decaens, Michel Jaquinod, Jérôme Boursier, Virginie Brun
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摘要

据估计,代谢功能障碍相关性脂肪性肝病(MASLD)影响着全球 30% 的人口,其发病率正随着肥胖的增加而上升。肝纤维化与死亡率密切相关,是代谢功能紊乱相关性脂肪肝最重要的临床参数。目前评估肝纤维化的方法是肝活检--这是一种有一定局限性的侵入性操作。因此,迫切需要一种可靠的非侵入性方法来诊断 MASLD 的早期阶段。我们利用基于质谱(MS)的定量蛋白质组学,对 158 份组织学特征明确的 MASLD 患者血浆样本进行了发现性研究。通过 ELISA 方法,在同一组群中筛选出不同含量的蛋白质进行验证。随后在一个独立的 MASLD 群体(n = 200)中对这些蛋白质进行了验证。从早期(F0-2)和晚期(F3-4)纤维化患者之间含量不同的 72 种蛋白质中,我们选择了胰岛素样生长因子结合蛋白复合物酸性易变亚基(ALS)和 Galectin-3 结合蛋白(Gal-3BP)进行进一步研究。在我们的验证队列中,ALS 和 Gal-3BP 的 AUROCs 和 95% CI 分别为 0.744 [0.673 - 0.816] 和 0.735 [0.661 - 0.81]。将 ALS 和 Gal-3BP 结合使用可改善对晚期肝纤维化的评估,AUROC 为 0.796 [0.731. 0.862]。在预测晚期肝纤维化方面,{ALS; Gal-3BP}模型超过了经典的纤维化面板。要证实 ALS 和 Gal-3BP 单独使用或与其他生物标记物结合使用对诊断肝纤维化的有用性,还需要对补充队列进行进一步研究。随着酶联免疫吸附测定法的问世,这些发现可以迅速应用于临床,为患者带来直接益处。
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Plasma ALS and Gal-3BP differentiate early from advanced liver fibrosis in MASLD patients
Metabolic dysfunction-associated steatotic liver disease (MASLD) is estimated to affect 30% of the world’s population, and its prevalence is increasing in line with obesity. Liver fibrosis is closely related to mortality, making it the most important clinical parameter for MASLD. It is currently assessed by liver biopsy – an invasive procedure that has some limitations. There is thus an urgent need for a reliable non-invasive means to diagnose earlier MASLD stages. A discovery study was performed on 158 plasma samples from histologically-characterised MASLD patients using mass spectrometry (MS)-based quantitative proteomics. Differentially abundant proteins were selected for verification by ELISA in the same cohort. They were subsequently validated in an independent MASLD cohort (n = 200). From the 72 proteins differentially abundant between patients with early (F0-2) and advanced fibrosis (F3-4), we selected Insulin-like growth factor-binding protein complex acid labile subunit (ALS) and Galectin-3-binding protein (Gal-3BP) for further study. In our validation cohort, AUROCs with 95% CIs of 0.744 [0.673 – 0.816] and 0.735 [0.661 – 0.81] were obtained for ALS and Gal-3BP, respectively. Combining ALS and Gal-3BP improved the assessment of advanced liver fibrosis, giving an AUROC of 0.796 [0.731. 0.862]. The {ALS; Gal-3BP} model surpassed classic fibrosis panels in predicting advanced liver fibrosis. Further investigations with complementary cohorts will be needed to confirm the usefulness of ALS and Gal-3BP individually and in combination with other biomarkers for diagnosis of liver fibrosis. With the availability of ELISA assays, these findings could be rapidly clinically translated, providing direct benefits for patients.
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来源期刊
Biomarker Research
Biomarker Research Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
15.80
自引率
1.80%
发文量
80
审稿时长
10 weeks
期刊介绍: Biomarker Research, an open-access, peer-reviewed journal, covers all aspects of biomarker investigation. It seeks to publish original discoveries, novel concepts, commentaries, and reviews across various biomedical disciplines. The field of biomarker research has progressed significantly with the rise of personalized medicine and individual health. Biomarkers play a crucial role in drug discovery and development, as well as in disease diagnosis, treatment, prognosis, and prevention, particularly in the genome era.
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