Clinical performance of an antibody-free assay for plasma Aβ42/Aβ40 to detect early alterations of Alzheimer’s disease in individuals with subjective cognitive decline

María Pascual‐Lucas(Fundacion Agencia Aragonesa para la Investigacion y el Desarrollo), José Antonio Allué(Grifols (Spain)), Leticia Sarasa(Grifols (Spain)), Noelia Fandos(Grifols (Spain)), Sergio Castillo(Grifols (Spain)), J. Terencio(Grifols (Spain)), Manuel Sarasa(Grifols (Spain)), Juan Pablo Tartari(Universitat Internacional de Catalunya), Ángela Sanabria(Instituto de Salud Carlos III), Lluís Tárraga(Instituto de Salud Carlos III), Agustı́n Ruiz(Instituto de Salud Carlos III), Marta Marquié(Instituto de Salud Carlos III), Sang Won Seo(Samsung Medical Center), Hyemin Jang(Samsung Medical Center), Merçé Boada(Instituto de Salud Carlos III), on behalf of the FACEHBI study group(Instituto de Salud Carlos III), N. Aguilera(Instituto de Salud Carlos III), Emilio Alarcón‐Martín(Samsung Medical Center), Montserrat Alegret(Samsung Medical Center), Sílvia Alonso-Lana(Samsung Medical Center), Marcelo L. Berthier(Instituto de Salud Carlos III), U. Bojayrin(Samsung Medical Center), Mar Buendía(Samsung Medical Center), Santiago Bullich(Grifols (Spain)), Francisco Campos, Amanda Cano(Universitat Internacional de Catalunya), Pilar Cañabate(Instituto de Salud Carlos III), L. Cañada(Instituto de Salud Carlos III), Claudia Cuevas(Samsung Medical Center), Itziar de Rojas(Samsung Medical Center), S. Diego, Ana Espinosa(Samsung Medical Center), Ester Esteban‐De Antonio, A. Gailhajenet, Asunción Garcı́a-Sánchez(Universitat Internacional de Catalunya), Philip Garcia(Samsung Medical Center), J.C. Juárez Giménez(Samsung Medical Center), Marta Gómez‐Chiari(Samsung Medical Center), M. Guitart(Samsung Medical Center), I. Hernández(Samsung Medical Center), Marta Ibarria, A. Lafuente(Samsung Medical Center), Núria Lleonart(Grifols (Spain)), F. Lomeña(Samsung Medical Center), E. Martín(Samsung Medical Center), M. Moreno, A.M. Morera(Instituto de Salud Carlos III), Laura Montrreal(Samsung Medical Center), N. Muñoz(Instituto de Salud Carlos III), Leire Narvaiza, A. Niñerola(Instituto de Salud Carlos III), A. B. Nogales(Instituto de Salud Carlos III), L. Núñez, Adelina Orellana(Samsung Medical Center), Gemma Ortega, Antonio Páez, Ana Pancho(Samsung Medical Center), E. Pelejà(Samsung Medical Center), Elsa Pérez, Alba Pérez‐Cordón, Andrés Perissinotti(Samsung Medical Center), Sílvia Preckler, Vanesa Pytel(Samsung Medical Center), Mario Ricciardi(Samsung Medical Center), Octavio Rodríguez‐Gómez(Samsung Medical Center), Núria Roé-Vellvé(Samsung Medical Center), Maribel Ramis(Samsung Medical Center), Maitée Rosende‐Roca(Samsung Medical Center), Susanna Seguer(Samsung Medical Center), Óscar Sotolongo‐Grau, Andrew Stephens(Samsung Medical Center), M. A. Tejero(Samsung Medical Center), M.D. Martínez del Valle Torres(Samsung Medical Center), Sergi Valero(Instituto de Salud Carlos III), Luis Vargas, Assumpta Vivas
Alzheimer s Research & Therapy
January 5, 2023
10.1186/s13195-022-01143-z
Cited by 39Open Access
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Abstract

BACKGROUND: Accessible and cost-effective diagnostic tools are urgently needed to accurately quantify blood biomarkers to support early diagnosis of Alzheimer's disease (AD). In this study, we investigated the ability of plasma amyloid-beta (Aβ)42/Aβ40 ratio measured by an antibody-free mass-spectrometric (MS) method, ABtest-MS, to detect early pathological changes of AD. METHODS: F-Florbetaben PET as the reference standard (cutoff for early amyloid deposition of 13.5 centiloids). Cross-validation was performed in an independent DPUK-Korean cohort. Additionally, associations of plasma Aβ42/Aβ40 with episodic memory performance and brain atrophy were assessed. RESULTS: The FACEHBI cohort at baseline included 200 healthy individuals with subjective cognitive decline (SCD), of which 36 (18%) were Aβ-PET positive. Plasma Aβ42/Aβ40 levels were significantly lower in Aβ-PET positive individuals (median [interquartile range, IQR], 0.215 [0.203-0.236]) versus Aβ-PET negative subjects (median [IQR], 0.261 [0.244-0.279]) (P < .001). Plasma Aβ42/Aβ40 was significantly correlated with Aβ-PET levels (rho = -0.390; P < .001) and identified Aβ-PET status with an area under the receiver operating characteristic curve (AUC) of 0.87 (95% confidence interval [CI], 0.80-0.93). A cutoff for the Aβ42/Aβ40 ratio of 0.241 (maximum Youden index) yielded a sensitivity of 86.1% and a specificity of 80.5%. These findings were cross-validated in an independent DPUK-Korean cohort (AUC 0.86 [95% CI 0.77-0.95]). Lower plasma Aβ42/Aβ40 ratio was associated with worse episodic memory performance and increased brain atrophy. Plasma Aβ42/Aβ40 at baseline predicted clinical conversion to mild cognitive impairment and longitudinal changes in amyloid deposition and brain atrophy at 2-year follow-up. CONCLUSIONS: This study suggests that plasma Aβ42/Aβ40, as determined by this MS-based assay, has potential value as an accurate and cost-effective tool to identify individuals in the earliest stages of AD, supporting its implementation in clinical trials, preventative strategies and clinical practice.

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