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The prodromal phase of hereditary spastic paraplegia type 4: the preSPG4 cohort study

遗传性痉挛性截瘫 医学 截瘫 痉挛的 队列 队列研究 儿科 内科学 物理医学与康复 遗传学 精神科 生物 脊髓 脑瘫 基因 表型
作者
Tim W. Rattay,Maximilian Völker,Maren Rautenberg,Christoph Keßler,Isabel Wurster,Natalie Winter,Tobias B. Haack,Tobias Lindig,Holger Hengel,Matthis Synofzik,Rebecca Schüle,Peter Martus,Lüdger Schöls
出处
期刊:Brain [Oxford University Press]
卷期号:146 (3): 1093-1102 被引量:12
标识
DOI:10.1093/brain/awac155
摘要

Abstract This cohort study aimed to characterize the prodromal phase of hereditary spastic paraplegia type 4 (SPG4) using biomarkers and clinical signs and symptoms that develop before manifest gait abnormalities. Fifty-six first-degree relatives at risk of developing SPG4 underwent blinded genotyping and standardized phenotyping, including the Spastic Paraplegia Rating Scale (SPRS), complicating symptoms, non-motor affection, Three-Minute Walk, and neurophysiological assessment. Automated MR image analysis was used to compare volumetric properties. CSF of 33 probands was analysed for neurofilament light chain (NfL), tau, and amyloid-β (Aβ). Thirty participants turned out to be SPAST mutation carriers, whereas 26 did not inherit a SPAST mutation. Increased reflexes, ankle clonus, and hip abduction weakness were more frequent in prodromal mutation carriers but were also observed in non-mutation carriers. Only Babinski's sign differentiated reliably between the two groups. Timed walk and non-motor symptoms did not differ between groups. Whereas most mutation carriers had total SPRS scores of 2 points or more, only two non-mutation carriers reached more than 1 point. Motor evoked potentials revealed no differences between mutation and non-mutation carriers. We found NfL but not tau or Aβ to rise in CSF of mutation carriers when approaching the time point of predicted disease manifestation. Serum NfL did not differ between groups. Volumetric MRI analyses did not reveal group differences apart from a smaller cingulate gyrus in mutation carriers. This study depicts subtle clinical signs which develop before gait abnormalities in SPG4. Long-term follow-up is needed to study the evolution of SPG4 in the prodromal stage and conversion into manifest disease. NfL in CSF is a promising fluid biomarker that may indicate disease activity in prodromal SPG4 but needs further evaluation in longitudinal studies.
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