Simple and reliable ALS diagnosis with blood tests

Simple and reliable ALS diagnosis with blood tests
Biomarker correlation to survival, survival analyses in clinical symptom onset and genotype groups, biomarker ratios and ALSFRS-R in ALS patients. (A) Correlation between plasma NFL and survival after symptom onset stratified by spinal and bulbar symptom onset. (B) Kaplan–Meier survival analysis for spinal onset versus bulbar onset ALS patients. (C) Correlation between plasma NFL and survival after symptom onset for participants in the total ALS cohort. (D) Kaplan–Meier survival analysis between patients with no known mutation, SOD1 mutation and C9orf72HRE mutation (p-value presented for overall comparisons). (E) Ratios and correlations between plasma NFL and CSF NFL stratified for spinal onset and bulbar onset ALS patients. (F) Correlation between CSF NFL and CSF pNFH for participants in the total ALS cohort. (G) Correlation between ALSFRS-R and plasma NFL in ALS patients. (H) Correlation between ALSFRS-R and survival after symptom onset in ALS patients. Credit: DOI: 10.1038/s41598-021-01499-6

Blood tests may enable more accurate diagnosis of ALS at an earlier stage of the disease. As described in a study by researchers at University of Gothenburg and Umeå University, it involves measuring the blood level of a substance that, as they have also shown, varies in concentration depending on which variant of ALS the patient has.

The study, published in Scientific Reports, include Fani Pujol-Calderón, postdoctoral fellow at Sahlgrenska Academy, University of Gothenburg, and Arvin Behzadi, doctoral student at Umeå University and medical intern at Örnsköldsvik Hospital, as shared first authors.

Currently, it is difficult to diagnose amyotrophic lateral sclerosis (ALS), the most common form of motor neuron disease, early in the course of the disease. Even after a prolonged investigation, there is a risk of misdiagnosis due to other diseases that may resemble ALS in early stages. Much would be gained from earlier correct diagnosis and, according to the researchers, the current findings look promising.

Neurofilaments—proteins with a special role in the cells and fibers of nerves—are the substances of interest. When the is damaged, neurofilaments leak into the cerebrospinal fluid (CSF) and in lower concetrations in blood compared to CSF. In their study, scientists at Umeå University and the University Hospital of Umeå, as well as at the University of Gothenburg and Sahlgrenska University Hospital in Gothenburg, demonstrated that CSF and blood levels of neurofilaments can differentiate ALS from other diseases that may resemble early ALS.

More sensitive methods of analysis

Compared with several other , previous studies have shown higher concentrations of neurofilaments in CSF in ALS. Measuring levels in the blood has previously been difficult since they occur at much lower concentrations compared to CSF. In recent years, however, new and more sensitive analytical methods have generated new scope for doing so.

The current study shows a strong association, in patients with ALS, between the quantity of neurofilaments in the blood and in CSF. The study is based on blood and CSF samples collected from 287 patients who had been referred to the Department of Neurology at the University Hospital of Umeå for investigation of possible motor neuron disease. After extensive investigation, 234 of these patients were diagnosed with ALS. These had significantly higher levels of neurofilaments in CSF and blood compared to patients who were not diagnosed with ALS.

Higher concentrations

Differences among various subgroups of ALS were also investigated and detected. Patients whose pathological symptoms started in the head and neck region had higher neurofilament concentrations in the blood and worse survival than patients whose disease onset began in an arm or a leg. The study has also succeeded in quantifying differences in blood levels of neurofilaments and survival for the two most common mutations associated to ALS.

"Finding suspected cases of ALS through a opens up completely new opportunities for screening and measuring neurofilaments in collected longitudinally enables easier quantification of treatment effects in clinical drug trials compared to longitudinal collection of CSF. Finding ALS early in the course may facilitate earlier administration of pharmaceutical treatment, before the muscles have atrophied," Arvin Behzadi says.

ALS is a neurodegenerative syndrome that leads to loss of nerve cells in both the brain and the spinal cord, resulting in muscle weakness and atrophy. Most of these patients die within two to four years after the symptom onset, but roughly one in ten survive more than ten years after the symptoms first appeared. Several genetic mutations have been associated to ALS. At present, there is no curative treatment. Nevertheless, the current drug available has been shown to prolong the survival in some ALS patients if it is administered in time.


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More information: Arvin Behzadi et al, Neurofilaments can differentiate ALS subgroups and ALS from common diagnostic mimics, Scientific Reports (2021). DOI: 10.1038/s41598-021-01499-6
Journal information: Scientific Reports

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