Abstract
Background The loss of neurological function is closely related to axonal damage. Neurofilament subunits are concentrated in neurons and axons and have emerged as promising biomarkers for neurodegeneration. Electrochemiluminescence (ECL) based assays are known to be of superior sensitivity and require less sample volume than conventional ELISAs. Methods We developed an ECL based solid-phase sandwich immunoassay to measure the neurofilament heavy chain protein (NfH SMI35) in CSF. We employed commercially available antibodies as previously used in a conventional ELISA (Petzold et al., 2003; Petzold and Shaw, 2007). The optimised and validated assay was applied in a reference cohort and defined patient groups. Results Analytical sensitivity (background plus three SD) of our assay was 2.4 pg/ml. The mean intra-assay coefficient of variation (CV) was 4.8% and the inter-assay CV 8.4%. All measured control and patient samples produced signals well above background. Patients with multiple sclerosis (MS) (median 46.2 pg/ml, n = 95), amyotrophic lateral sclerosis (ALS) (160.1 pg/ml, n = 50), mild cognitive impairment/Alzheimer's disease (MCI/AD) (65.6 pg/ml, n = 20), Guillain–Barre syndrome (GBS) (91.0 pg/ml, n = 20) or subarachnoid hemorrhage (SAH) (345.0 pg/ml, n = 20) had higher CSF NfH SMI35 values than the reference cohort (27.1 pg/ml, n = 73, p < 0.0001 for each comparison). Conclusion The new ECL based assay for NfH SMI35 in CSF is superior in terms of sensitivity, precision and accuracy to previously published methods (Petzold et al., 2003; Shaw et al., 2005; Teunissen et al., 2009). The improved performance and small sample volume requirement qualify this method in experimental settings and clinical trials designed to perform a number of tests on limited amounts of material.
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