Annals of Clinical and Translational Neurology (Apr 2022)

Development of an age‐adjusted model for blood neurofilament light chain

  • Christopher Harp,
  • Gian‐Andrea Thanei,
  • Xiaoming Jia,
  • Jens Kuhle,
  • David Leppert,
  • Sabine Schaedelin,
  • Pascal Benkert,
  • H‐Christian vonBüdingen,
  • Robert Hendricks,
  • Ann Herman

DOI
https://doi.org/10.1002/acn3.51524
Journal volume & issue
Vol. 9, no. 4
pp. 444 – 453

Abstract

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Abstract Objective To develop an age‐adjustment model for neurofilament light chain (NfL), an emerging injury marker in patients with a range of neurologic conditions including multiple sclerosis (MS). Methods Serum and plasma samples were collected from a healthy donor (HD) cohort of 118 individuals aged 24 to 66 years, 90 patients with relapsing MS (RMS) and 22 patients with progressive MS (PMS). Serum and plasma samples were assessed for NfL using the SIMOA assay (Quanterix NfL Advantage Kit™). A log‐linear model was used to evaluate the relationship between NfL and age and to calculate age‐adjusted NfL levels. Results Higher serum and plasma NfL levels were significantly associated with increasing HD age. Log‐transformation of blood NfL levels reduced heteroscedasticity and skewness. A log‐linear model enabled adjustment for age‐related increase in serum and plasma NfL levels (2.3% [95% CI, 1.6–2.9] and 2.6% [95% CI, 1.3–3.3] per year, respectively). Following age adjustment, NfL did not show significant association with HD sex or ethnicity. While unadjusted serum NfL levels were elevated in patients with PMS (mean age 56 years) compared with those with RMS (mean age 37 years), age‐adjusted NfL levels did not differ. Interpretation A log‐linear, age adjustment model was developed to enable comparison of NfL levels across populations with different ages. While additional data and evidence are needed for patient‐level adoption, this could be a valuable tool for interpreting NfL levels across a range of patient groups with neurologic conditions.