Plasma neurofilament light in Huntington's disease: A marker for disease onset, but not symptom progression

To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy. 98 participants (33 control, 26 PM, 39 HD), underwent blood sample colle...

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Published in	Parkinsonism & related disorders Vol. 87; pp. 32 - 38
Main Authors	Parkin, Georgia M., Corey-Bloom, Jody, Snell, Chase, Castleton, Jordan, Thomas, Elizabeth A.
Format	Journal Article
Language	English
Published	England Elsevier Ltd 01.06.2021
Subjects	Adult Aged Aged, 80 and over Biomarker Biomarkers - blood Blood Cohort Studies Disease Progression Female Humans Huntington Disease - blood Huntington Disease - diagnosis Huntington's disease Male Middle Aged Neurofilament light Neurofilament Proteins - blood Plasma Prodromal Symptoms Young Adult Neurofilament light Plasma Biomarker Huntington's disease Blood
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ISSN	1353-8020 1873-5126 1873-5126
DOI	10.1016/j.parkreldis.2021.04.017

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Abstract	To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy. 98 participants (33 control, 26 PM, 39 HD), underwent blood sample collection and clinical assessment, using both UHDRS and non-UHDRS measures, at one academic HD Center. Years to onset (YTO), probability of disease onset in 5 years, and predicted years until 60% onset probability were also calculated. NfL levels were measured using a Meso Scale Discovery assay. Cohorts differed by age. NfL levels differed significantly across diagnostic groups and were significantly correlated with age. Age-adjusted NfL levels were not correlated with clinical measures in either HD or PM cohorts, but were correlated when cohorts were combined. In PM subjects, NfL levels correlated with YTO, probability of onset in 5 years, and years until 60% onset probability. Using ROC analysis, a NfL cut-point of <53.15 pg/ml distinguished HD from control; <74.84 pg/ml distinguished HD from PM. These findings implicate plasma NfL as a peripheral prognostic marker for premanifest-HD. Notably, we show that significant correlations between NfL and clinical symptoms are detected only when PM + HD subjects are combined, but not within HD subjects alone. To date, prior studies have investigated the clinical usefulness of NfL exclusively in merged PM + HD cohorts. Our data suggests a biasing of these previous correlations, and hence potentially limited usefulness of plasma NfL in monitoring HD symptom progression, for example, in clinical trials. •Plasma NfL is correlated with years to onset in premanifest HD (PM).•Plasma NfL levels are significantly elevated following HD symptom onset.•Plasma NfL is not correlated with symptom progression after HD symptom onset.•Past studies of the mutation-positive cohort did not consider PM and HD separately.•Plasma NfL may not be a useful biomarker in clinical trials of manifest HD subjects.
AbstractList	To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy. 98 participants (33 control, 26 PM, 39 HD), underwent blood sample collection and clinical assessment, using both UHDRS and non-UHDRS measures, at one academic HD Center. Years to onset (YTO), probability of disease onset in 5 years, and predicted years until 60% onset probability were also calculated. NfL levels were measured using a Meso Scale Discovery assay. Cohorts differed by age. NfL levels differed significantly across diagnostic groups and were significantly correlated with age. Age-adjusted NfL levels were not correlated with clinical measures in either HD or PM cohorts, but were correlated when cohorts were combined. In PM subjects, NfL levels correlated with YTO, probability of onset in 5 years, and years until 60% onset probability. Using ROC analysis, a NfL cut-point of <53.15 pg/ml distinguished HD from control; <74.84 pg/ml distinguished HD from PM. These findings implicate plasma NfL as a peripheral prognostic marker for premanifest-HD. Notably, we show that significant correlations between NfL and clinical symptoms are detected only when PM + HD subjects are combined, but not within HD subjects alone. To date, prior studies have investigated the clinical usefulness of NfL exclusively in merged PM + HD cohorts. Our data suggests a biasing of these previous correlations, and hence potentially limited usefulness of plasma NfL in monitoring HD symptom progression, for example, in clinical trials. •Plasma NfL is correlated with years to onset in premanifest HD (PM).•Plasma NfL levels are significantly elevated following HD symptom onset.•Plasma NfL is not correlated with symptom progression after HD symptom onset.•Past studies of the mutation-positive cohort did not consider PM and HD separately.•Plasma NfL may not be a useful biomarker in clinical trials of manifest HD subjects. To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy. 98 participants (33 control, 26 PM, 39 HD), underwent blood sample collection and clinical assessment, using both UHDRS and non-UHDRS measures, at one academic HD Center. Years to onset (YTO), probability of disease onset in 5 years, and predicted years until 60% onset probability were also calculated. NfL levels were measured using a Meso Scale Discovery assay. Cohorts differed by age. NfL levels differed significantly across diagnostic groups and were significantly correlated with age. Age-adjusted NfL levels were not correlated with clinical measures in either HD or PM cohorts, but were correlated when cohorts were combined. In PM subjects, NfL levels correlated with YTO, probability of onset in 5 years, and years until 60% onset probability. Using ROC analysis, a NfL cut-point of <53.15 pg/ml distinguished HD from control; <74.84 pg/ml distinguished HD from PM. These findings implicate plasma NfL as a peripheral prognostic marker for premanifest-HD. Notably, we show that significant correlations between NfL and clinical symptoms are detected only when PM + HD subjects are combined, but not within HD subjects alone. To date, prior studies have investigated the clinical usefulness of NfL exclusively in merged PM + HD cohorts. Our data suggests a biasing of these previous correlations, and hence potentially limited usefulness of plasma NfL in monitoring HD symptom progression, for example, in clinical trials. To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy.OBJECTIVETo investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL cut-point could distinguish PM from HD patients with reasonable accuracy.98 participants (33 control, 26 PM, 39 HD), underwent blood sample collection and clinical assessment, using both UHDRS and non-UHDRS measures, at one academic HD Center. Years to onset (YTO), probability of disease onset in 5 years, and predicted years until 60% onset probability were also calculated. NfL levels were measured using a Meso Scale Discovery assay.METHOD98 participants (33 control, 26 PM, 39 HD), underwent blood sample collection and clinical assessment, using both UHDRS and non-UHDRS measures, at one academic HD Center. Years to onset (YTO), probability of disease onset in 5 years, and predicted years until 60% onset probability were also calculated. NfL levels were measured using a Meso Scale Discovery assay.Cohorts differed by age. NfL levels differed significantly across diagnostic groups and were significantly correlated with age. Age-adjusted NfL levels were not correlated with clinical measures in either HD or PM cohorts, but were correlated when cohorts were combined. In PM subjects, NfL levels correlated with YTO, probability of onset in 5 years, and years until 60% onset probability. Using ROC analysis, a NfL cut-point of <53.15 pg/ml distinguished HD from control; <74.84 pg/ml distinguished HD from PM.RESULTSCohorts differed by age. NfL levels differed significantly across diagnostic groups and were significantly correlated with age. Age-adjusted NfL levels were not correlated with clinical measures in either HD or PM cohorts, but were correlated when cohorts were combined. In PM subjects, NfL levels correlated with YTO, probability of onset in 5 years, and years until 60% onset probability. Using ROC analysis, a NfL cut-point of <53.15 pg/ml distinguished HD from control; <74.84 pg/ml distinguished HD from PM.These findings implicate plasma NfL as a peripheral prognostic marker for premanifest-HD. Notably, we show that significant correlations between NfL and clinical symptoms are detected only when PM + HD subjects are combined, but not within HD subjects alone. To date, prior studies have investigated the clinical usefulness of NfL exclusively in merged PM + HD cohorts. Our data suggests a biasing of these previous correlations, and hence potentially limited usefulness of plasma NfL in monitoring HD symptom progression, for example, in clinical trials.CONCLUSIONSThese findings implicate plasma NfL as a peripheral prognostic marker for premanifest-HD. Notably, we show that significant correlations between NfL and clinical symptoms are detected only when PM + HD subjects are combined, but not within HD subjects alone. To date, prior studies have investigated the clinical usefulness of NfL exclusively in merged PM + HD cohorts. Our data suggests a biasing of these previous correlations, and hence potentially limited usefulness of plasma NfL in monitoring HD symptom progression, for example, in clinical trials.
Author	Thomas, Elizabeth A. Castleton, Jordan Parkin, Georgia M. Snell, Chase Corey-Bloom, Jody
AuthorAffiliation	c Institute for Interdisciplinary Salivary Bioscience Research, University of California Irvine, Irvine, CA, USA a Department of Epidemiology, University of California Irvine, Irvine, CA, USA b Department of Neurosciences, University of California San Diego, San Diego, CA, USA
AuthorAffiliation_xml	– name: a Department of Epidemiology, University of California Irvine, Irvine, CA, USA – name: c Institute for Interdisciplinary Salivary Bioscience Research, University of California Irvine, Irvine, CA, USA – name: b Department of Neurosciences, University of California San Diego, San Diego, CA, USA
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Keywords	Neurofilament light Plasma Biomarker Huntington's disease Blood
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Snippet	To investigate whether plasma NfL levels correlate with clinical symptom severity in premanifest (PM) and manifest HD (HD) individuals, and whether a NfL...
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SubjectTerms	Adult Aged Aged, 80 and over Biomarker Biomarkers - blood Blood Cohort Studies Disease Progression Female Humans Huntington Disease - blood Huntington Disease - diagnosis Huntington's disease Male Middle Aged Neurofilament light Neurofilament Proteins - blood Plasma Prodromal Symptoms Young Adult
Title	Plasma neurofilament light in Huntington's disease: A marker for disease onset, but not symptom progression
URI	https://www.clinicalkey.com/#!/content/1-s2.0-S1353802021001504 https://dx.doi.org/10.1016/j.parkreldis.2021.04.017 https://www.ncbi.nlm.nih.gov/pubmed/33940564 https://www.proquest.com/docview/2522184562 https://pubmed.ncbi.nlm.nih.gov/PMC9083556
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