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Serum biomarkers at disease onset for personalized therapy in multiple sclerosis

医学 扩大残疾状况量表 内科学 多发性硬化 比例危险模型 麦当劳标准 胃肠病学 免疫学
作者
Enric Monreal,José Ignacio Fernández-Velasco,Roberto Álvarez‐Lafuente,Susana Sainz de la Maza,María Isabel García-Sánchez,Sara Llufriú,Bonaventura Casanova,Manuel Comabella,Sergio Martínez‐Yélamos,Daniela Galimberti,Lluís Ramió‐Torrentà,María Luisa Martínez‐Ginés,Yolanda Aladro,Lucía Ayuso,José Rodríguez,Luís Brieva,Noelia Villarrubia,Sara Eichau,Javier Zamora,Alexander Rodero-Romero,Mercedes Espiño,Yolanda Blanco,Albert Saiz,Xavier Montalbán,Mar Tintoré,María Inmaculada Domínguez‐Mozo,Juan Pablo Cuello,Lucía Romero,Laura Ghezzi,Belén Pilo de la Fuente,Francisco Pérez‐Miralles,Ana Quiroga‐Varela,Lluïsa Rubio,Fernando Rodríguez‐Jorge,Juan Luis Chico‐García,Raquel Sainz-Amo,Jaime Masjuán,Lucienne Costa‐Frossard,Luisa María Villar
出处
期刊:Brain [Oxford University Press]
标识
DOI:10.1093/brain/awae260
摘要

Abstract The potential of combining serum neurofilament light chain (sNfL) and glial fibrillary acidic protein (sGFAP) levels to predict disability worsening in multiple sclerosis (MS) remains underexplored. We aimed to investigate whether sNfL and sGFAP values identify distinct subgroups of patients according to the risk of disability worsening and their response to disease-modifying treatments (DMTs). This multicentre study, conducted across thirteen European hospitals, spanned from July 15, 1994, to August 18, 2022, with follow-up until September 26, 2023. We enrolled MS patients who had serum samples collected within 12 months from disease onset and before initiating DMTs. Multivariable regression models were used to estimate the risk of relapse-associated worsening (RAW), progression independent of relapse activity (PIRA), and Expanded Disability Status Scale (EDSS) score of 3. Of the 725 patients included, median age was 34.2 years (IQR, 27.6–42.4), and 509 patients (70.2%) were female. Median follow-up duration was 6.43 years (IQR, 4.65–9.81). Higher sNfL values associated with an elevated risk of RAW (HR of 1.45; 95% CI 1.19–1.76; P < 0.001), PIRA (HR of 1.43; 95% CI 1.13–1.81; P = 0.003), and reaching an EDSS of 3 (HR of 1.55; 95% CI 1.29–1.85; P < 0.001). Moreover, higher sGFAP levels were linked to a higher risk of achieving an EDSS score of 3 (HR of 1.36; 95% CI 1.06–1.74; P = 0.02) and, in patients with low sNfL values, to PIRA (HR of 1.86; 95% CI 1.01–3.45; P = 0.04). We further examined the combined effect of sNfL and sGFAP levels. Patients with low sNfL and sGFAP values (NLGL) exhibited a low risk of all outcomes and served as reference. Untreated patients with high sNfL levels showed a higher risk of RAW, PIRA, and reaching an EDSS of 3. Injectable or oral DMTs reduced the risk of RAW in these patients but failed to mitigate the risk of PIRA and reaching an EDSS of 3. Conversely, high-efficacy DMTs counteracted the heightened risk of these outcomes, except for the risk of PIRA in patients with high sNfL and sGFAP levels. Patients with low sNfL and high sGFAP values (NLGH) showed an increased risk of PIRA and achieving an EDSS of 3, which remained unchanged with either high-efficacy or other DMTs. In conclusion, evaluating sNfL and sGFAP levels at disease onset in MS may identify distinct phenotypes associated with diverse immunological pathways of disability acquisition and therapeutic response.
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