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    Is the phenotype designation by PSP-MDS criteria stable throughout the disease course and consistent with tau distribution?

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    Date
    2022
    Author
    Sánchez Ruiz de Gordoa, Javier Upna Orcid
    Zelaya Huerta, María Victoria Upna Orcid
    Tellechea-Aramburo, Paula 
    Acha Santamaría, Blanca Upna Orcid
    Roldán, Miren 
    Lopez Molina, Carlos 
    Coca, Valle 
    Galbete Jiménez, Arkaitz Upna Orcid
    Mendioroz, Maite 
    Erro, M. Elena 
    Version
    Acceso abierto / Sarbide irekia
    Type
    Artículo / Artikulua
    Version
    Versión publicada / Argitaratu den bertsioa
    Impact
     
     
     
    10.3389/fneur.2022.827338
     
     
     
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    Abstract
    Introduction: the MDS-PSP criteria have shown high sensitivity for the PSP diagnosis, but do not discriminate the phenotype diversity. Our purpose was to search for anatomopathological differences among PSP phenotypes resulting from the application of the MDS-PSP criteria comparing with the previous ones. Methods: thirty-four PSP cases from a single brain bank were retrospectively classified acco ... [++]
    Introduction: the MDS-PSP criteria have shown high sensitivity for the PSP diagnosis, but do not discriminate the phenotype diversity. Our purpose was to search for anatomopathological differences among PSP phenotypes resulting from the application of the MDS-PSP criteria comparing with the previous ones. Methods: thirty-four PSP cases from a single brain bank were retrospectively classified according to the criteria used by Respondek et al. in 2014 and the PSP-MDS criteria at 3 years (MDS-3y), 6 years (MDS-6y) and at the last clinical evaluation before death (MDS-last). Semiquantitative measurement of total, cortical and subcortical tau load was compared. For comparative analysis, PSP-Richardson syndrome and PSP postural instability were grouped (PSP-RS/PI) as well as the PSP atypical cortical phenotypes (PSP-Cx). Results: applying the Respondek's criteria, PSP phenotypes were distributed as follow: 55.9% PSP-RS/PI, 26.5% PSP-Cx, 11.8% PSP-Parkinsonism (PSP-P), and 5.9% PSP-Cerebellum. PSP-RS/PI and PSP-Cx had a higher total tau load than PSP-P; PSP-Cx showed a higher cortical tau load than PSP-RS/PI and PSP-P; and PSP-RS/PI had a higher subcortical tau load than PSP-P. Applying the MDS-3y, MDS-6y and MDS-last criteria; the PSP-RS/PI group increased (67.6, 70.6 and 70.6% respectively) whereas the PSP-Cx group decreased (8.8, and 8.8 and 11.8%). Then, only differences in total and subcortical tau burden between PSP-RS/PI and PSP-P were observed. Interpretation: after the retrospective application of the new MDS-PSP criteria, total and subcortical tau load is higher in PSP-RS/PI than in PSP-P whereas no other differences in tau load between phenotypes were found, as a consequence of the loss of phenotypic diversity. [--]
    Subject
    Clinical-pathological correlation, Phenotypes, Progressive supranuclear palsy (PSP), PSP-MDS criteria, Tau protein load, Tauopathies
     
    Publisher
    Frontiers Media
    Published in
    Frontiers in Neurology, 2022, 13
    Departament
    Universidad Pública de Navarra. Departamento de Estadística, Informática y Matemáticas / Nafarroako Unibertsitate Publikoa. Estatistika, Informatika eta Matematikak Saila
     
    Publisher version
    https://doi.org/10.3389/fneur.2022.827338
    URI
    https://hdl.handle.net/2454/43365
    Appears in Collections
    • Artículos de revista DAC - AKS Aldizkari artikuluak [81]
    • Artículos de revista - Aldizkari artikuluak [4588]
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