Plasma Neurofilament Light Chain and Clinical Diagnosis in Frontotemporal Dementia Syndromes

被引:6
|
作者
Ooi, Suyi [1 ,2 ,3 ,4 ]
Patel, Sheila K. [4 ]
Eratne, Dhamidhu [4 ,5 ,6 ,7 ]
Kyndt, Christopher [1 ,2 ,3 ]
Reidy, Natalie [1 ]
Lewis, Courtney [1 ,5 ,6 ,7 ]
Lee, Sarah C. M. [2 ,9 ]
Darby, David [1 ,2 ,3 ,8 ]
Brodtmann, Amy [1 ,2 ,3 ,4 ]
机构
[1] Eastern Hlth, Eastern Cognit Disorders Clin, Box Hill, Vic, Australia
[2] Monash Univ, Fac Med Nursing & Hlth Sci, Eastern Hlth Clin Sch, Eastern Clin Res Unit, Melbourne, Vic, Australia
[3] Royal Melbourne Hosp, Dept Neurol, Parkville, Vic, Australia
[4] Florey Inst Neurosci & Mental Hlth, Parkville, Vic, Australia
[5] Royal Melbourne Hosp, Neuropsychiat, Parkville, Vic, Australia
[6] Royal Melbourne Hosp, Melbourne Neuropsychiat Ctr, Parkville, Vic, Australia
[7] Univ Melbourne, Parkville, Vic, Australia
[8] Alfred Hlth, Dept Neurol, Prahran, Vic, Australia
[9] Calvary Hlth Care Bethlehem, Parkdale, Vic, Australia
关键词
Biomarker; frontotemporal dementia; neurofilament light; phenocopy; primary progressive aphasia; AMYOTROPHIC-LATERAL-SCLEROSIS; ALZHEIMERS-DISEASE; PROGRESSIVE APHASIA; TEMPORAL VARIANT; PATHOLOGY; BLOOD;
D O I
10.3233/JAD-220272
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
Background: Frontotemporal dementia (FTD) syndromes, mimics, phenocopy (phFTD), and slowly progressive behavioral variant FTD (bvFTD) can be difficult to distinguish clinically. Biomarkers such as neurofilament light chain (NfL) may be helpful. Objective: To study plasma NfL levels in people with FTD syndromes and determine if plasma NfL can distinguish between FTD syndromes and phFTD. Methods: Plasma NfL levels were estimated using both Simoa (R) Quanterix HD-XT and SR-XT machines grouped via final diagnosis after investigation and review. Results: Fifty participants were studied: bvFTD = 20, semantic variant FTD (svFTD) = 11, non-fluent variant FTD (nfvFTD) = 9, FTD with motor neuron disease (MND) = 4, phFTD = 2, slow progressors = 3, FTD mimic = 1, mean age 67.2 (SD 8.4) years. NfL levels were significantly higher in the FTD group compared to phenocopy group (p = 0.003). Median NfL (IQR) pg/mL was comparable in the FTD syndromes: bvFTD 41.10 (50.72), svFTD 44.38 (16.61), and nfvFTD 42.61 (22.93), highest in FTD with MND 79.67 (45.32) and lowest in both phFTD 13.99 (0.79) and slow progressors 17.97 (3.62). Conclusion: Plasma NfL appears to differentiate FTD syndromes and mimics. However, a lower NfL may predict a slower, but not necessarily absence of neurodegeneration, and therefore appears limited in distinguishing slow progressors from FTD phenocopies. Larger numbers of patients from all clinical groups are required to strengthen diagnostic utility.
引用
收藏
页码:1221 / 1231
页数:11
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