Submitted:
08 June 2026
Posted:
11 June 2026
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Abstract
Keywords:
- • Handheld Vibration applied to the upper limb significantly reduces transmission along reflex pathways within the spinal cord. H-reflex amplitude was reduced by 15.7%, and middle-latency cutaneous reflexes by 20%.
- • Handheld Vibration does not alter the excitability of the corticospinal pathway (the pathway from the brain to the muscle). Motor responses to TMS were unchanged.
- • The most likely mechanism is presynaptic inhibition — vibration appears to dampen incoming sensory signals before they can drive the motor neuron, rather than acting on the brain itself.
- • These findings have direct implications for rehabilitation. Conditions such as stroke, spinal cord injury, multiple sclerosis and cerebral palsy involve excessive spinal reflex activity (spasticity). Upper limb vibration may be a low-cost, drug-free way of reducing that activity within a rehabilitation session, complementing physiotherapy and other interventions.
- UK rehabilitation services (NHS, charities and private providers) should explore vibrotactile stimulation as a low-cost, non-pharmacological adjunct to conventional therapy for patients with spasticity following stroke, spinal cord injury or multiple sclerosis.
- UK research funders should support follow-on clinical studies to test these laboratory findings in patient populations and to identify the optimal parameters of vibration (frequency, amplitude, duration) for different conditions.
- Policymakers should consider the potential cost-saving and quality-of-life benefits of evidence-based vibration therapy as part of integrated rehabilitation pathways.
1. Background and UK Context
1.1. Why Vibration Therapy Matters
1.2. The UK Rehabilitation Challenge
1.3. The Scientific Gap Addressed by This Fellowship
2. Aims and Objectives of the Fellowship
2.1. Primary Objective
2.2. Secondary Objectives
- To contribute to ongoing neurophysiological research at the host laboratory, applying my skills in biomedical engineering, software programming and signal processing to projects beyond my own.
- To plan and, where possible, to begin a substantive collaborative experiment using TMS to investigate the effects of upper limb vibration on the human nervous system.
- To establish a longer-term research collaboration with the host laboratory, with the goal of pursuing further joint research projects and grant applications after the Fellowship period.
3. Purpose of This Report
4. Approach: The Fellowship Visit
4.1. Host Institution and Laboratory
4.2. Duration and Structure
- Weeks 1–2: Foundations. Reading, lab tutorials and observation. Understanding the theory, neurophysiological underpinnings, advantages and limitations of TMS; learning the safety screening procedures; observing experiments being run by other members of the laboratory.
- Weeks 3–6: Experimental work. Hands-on TMS practice; design of the upper-limb vibration experiment; integration of my purpose-built vibration device into the laboratory’s experimental rig; participant recruitment and screening; collection of data from the full participant cohort; ongoing involvement in other neurophysiological projects to which I contributed software and signal-processing expertise.
- Weeks 7–8: Analysis and forward planning. Initial data analysis; review of the experiment as a whole; design of follow-on experiments; agreement of a longer-term collaboration plan with the host laboratory; outline of the manuscript that would later be published in Frontiers in Human Neuroscience.
4.3. The Experimental Study
- • H-reflexes (with and without conditioning) evoked by electrical stimulation of the median nerve, to probe the excitability of spinal reflex pathways and the degree of presynaptic inhibition acting on them.
- • Cutaneous reflexes evoked by electrical stimulation of the superficial radial nerve, to probe how sensory information from the skin is integrated by the spinal cord.
- • Motor evoked potentials (MEPs) elicited by Transcranial Magnetic Stimulation of the motor cortex, to probe the excitability of the corticospinal pathway from brain to muscle.
5. Findings
5.1. Acquiring TMS as a Neurophysiological Investigation Tool
5.2. Designing an Experiment to Distinguish Spinal from Corticospinal Effects
5.3. Vibration Inhibits Spinal Reflex Pathways
5.4. Handheld Vibration Does Not Alter Corticospinal Excitability
5.5. The Likely Mechanism: Presynaptic Inhibition
5.6. Clinical and Rehabilitation Implications for the UK
5.6.1. Stroke Survivors
5.6.2. People Living with Spinal Cord Injury
5.6.3. People with Multiple Sclerosis
5.6.4. Other Groups
5.6.5. Implementation: Opportunities and Challenges
5.7. Lessons in Interdisciplinary Collaboration
6. Conclusion
7. Recommendations
7.1. To UK Rehabilitation Services and Clinicians
7.2. To UK Research Funders
7.3. To UK Universities and Research Institutions
7.4. To UK Manufacturers and Standards Bodies
7.5. To UK Policymakers and Commissioners
8. Next Steps
- Patient studies. The most important single next step is a programme of well-designed studies in patient populations. The first targets are likely to be people with stroke, cerebral palsy multiple sclerosis and spinal injury. Some of this work has already been initiated, in stroke [7], cerebral palsy [8,9], spinal injury (review) [10]. I am actively pursuing collaborations with UK and international clinical centres and patient organisations to make these studies possible.
- Mechanism studies. Further mechanistic work is needed to confirm presynaptic inhibition as the principal mechanism, to test for postsynaptic contributions, and to investigate whether longer or repeated exposure to vibration produces lasting (plastic) changes in spinal circuits. Such changes would substantially strengthen the case for vibration as a rehabilitation tool.
- Engagement and dissemination. I will continue to share these findings with clinicians, charities, patient groups and policymakers across the UK. I welcome contact from anyone working in this area or interested in collaboration; my contact details are on the inside cover of this report. Engagement with UK and international, clinicians [13] and researchers [14] has already led to growing collaborative work in neurorehabilitation.
Abbreviations and Glossary
Acknowledgments
Appendix A — Host Institution and Mentor
References
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