RecruitingNCT05663008

Impairments of Neuro-muscular Communication in Motor-Neuron Disease: A Bio-Marker for Early and Personalised Diagnosis

Sponsor

University of Dublin, Trinity College

Enrollment

400 participants

Start Date

Oct 1, 2015

Study Type

OBSERVATIONAL

Conditions

Spinal Muscular Atrophy ALS (Amyotrophic Lateral Sclerosis)Postpoliomyelitis Syndrome

Summary

Motor neuron disease (MND) or ALS is a nervous system disease. ALS leads to a loss of movement ability that eventually leads to death. At the moment, there is no known treatment for ALS. Early diagnosis in individuals improves clinical care and facilitates timely entry into clinical trials. However, current methods for diagnosis are primarily clinical, and to date, no cost-effective biomarkers have been developed. Our objective is to identify a robust non-invasive neurophysiological-based system that can be used both as a biomarker of disease onset, and a measurement of progression using quantitative EEG and surface EMG (bipolar and high-density). The investigators postulate that analysing the joint recordings of EEG and EMG (bipolar or high-density) can give measures that better distinguish healthy people and ALS patient subgroups and that the findings can be developed as biomarkers of early diagnosis and disease progression.

Eligibility

Min Age: 18 Years

Inclusion Criteria6

Healthy Volunteers:
age and gender-matched to patient groups
the intact physical ability to take part in the experiment.
Patients:
Diagnosis of ALS, PLS, PMA, SMA, Polio or MS
capable of providing informed consent.

Exclusion Criteria8

Healthy Controls:
History of neuromuscular
neurological or active psychiatric disease disease
history of reaction or allergy to recording environments, equipment and the recording gels.
Patients:
the presence of active psychiatric disease
any medical condition associated with severe neuropathy (e.g. poorly controlled diabetes).
History of reaction or allergy to recording environments, equipment and the recording gels.

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Interventions

PROCEDURE128 electrode electroencephalography (EEG), Bipolar surface electromyography (sEMG), High-density electromyography (HD-EMG)

128 electrode EEG and 8 bipolar EMG or HD-EMG will be noninvasively recorded from electrodes placed in a montage over the scalp and arm muscles while the participant is resting or performing tasks designed to engage specific cortical networks of interest (cognitive, behavioural, motor and sensory)

Locations(1)

Academic Unit of Neurology, Trinity College Dublin, The University of Dublin

Dublin, Leinster, Ireland

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NCT05663008

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