Safety and Efficacy of Transcranial Electromagnetic Treatment Against Alzheimer's Disease

Not Applicable

Completed

• Conditions: Alzheimer Disease, Late Onset; Alzheimer Disease
• Interventions: Device: MemorEM 1000

• Registration Number: NCT02958930
• Lead Sponsor: NeuroEM Therapeutics, Inc.

Brief Summary

The purpose of this study is to determine the safety and initial efficacy of Transcranial Electromagnetic Treatment (TEMT) in patients with mild/moderate Alzheimer's Disease. Throughout a 2-month treatment period, patients will be evaluated for cognitive performance, brain energy utilization, functional brain imaging, and blood/cerebrospinal fluid (CSF) markers for Alzheimer's Disease. Since all patients will receive TEMT, each patient's baseline measurements will serve as their own control for any treatment effects.

Detailed Description

There is currently no effective therapeutic to stabilize or reverse the cognitive impairment of Alzheimer's Disease (AD) and related dementias. Clinical trials with drugs have been unsuccessful because the wrong therapeutic target/species were selected, because drugs have great difficulty traversing the blood-brain barrier and getting into neurons, and/or because drugs largely have only a single mechanism of action. Since ever-increasing experimental evidence indicates that the toxic forms of both beta-amyloid and tau are the soluble "oligomeric" species of these two proteins, therapeutics to disaggregate these oligomers within neurons represent perhaps the best chance for attaining cognitive benefit in AD patients.

Pre-clinical studies performed by the Sponsor and his collaborators have demonstrated that AD transgenic mice treated daily with electromagnetic waves in the radiofrequency (RF) range are protected from cognitive impairment or show a reversal of pre-existing cognitive impairment. These cognitive benefits appear to be due primarily to two complimentary mechanisms: 1) disaggregation of toxic protein oligomers within neurons, and 2) mitochondrial enhancement to increase energy metabolism. Moreover, no deleterious effects of treatment over many months have been observed in these pre-clinical studies.

In order to provide similar treatment to mild/moderate Alzheimer's patients clinically, NeuroEM Therapeutics has developed a unique head device that provides electromagnetic (RF) treatment to the entire human forebrain at levels similar to those that provided cognitive benefits in pre-clinical studies. Using the MemorEM 1000 head device in the present Phase I trial, AD patients receive twice daily 1-hour treatments in-home, as administered by their caregiver. The device allows for the patient to have complete mobility for moving throughout their home.

A comprehensive array of markers will be analyzed both during and following the 2-month treatment period, with baseline (pre-treatment) values serving as controls. Cognitive safety and efficacy will be evaluated using a variety of cognitive assessments including ADAS-cog (Primary), and secondary cognitive measures including ADCS-ADL, Rey AVLT, Trails A \& B, Digit span, and clock draw tasks. Treatment effects on brain energy metabolism will be determine by FDG-PET scans, while treatment effects on brain functional connectivity will be determined through both resting state MRI and Diffusion Tensor Imaging. Also being assessed are the effects of treatment on various beta-amyloid and tau protein species (e.g., monomers, oligomers) in both blood and CSF. Safety of the treatment will be monitored by regular Adverse Events Assessment, physiologic monitoring, and patient daily diaries maintained by the caregiver.

Expected Results: The investigators expect that 2-months of daily electromagnetic (RF) treatment will not present any significant side effects or safety issues. The investigators further expect that cognitive measures will be stable and/or improve by the end of treatment. In addition, the investigators anticipate that brain functional connectivity may be improved and that enhanced brain metabolism (FDG-PET) will occur. Changes in blood/CSF levels of various beta-amyloid and tau species are also anticipated.

Study Timeline

• Study First Submitted: 2016-11-01
• Study First Submitted QC: 2016-11-07
• Study First Posted: 2016-11-08
• Study Start: 2017-10-01
• Primary Completion: 2019-01-04
• Study Completion: 2019-01-11
• Status Verified: 2019-04
• Last Update Submitted: 2019-04-22
• Last Update Posted: 2019-04-23

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 8

Inclusion Criteria

• Patients diagnosed with mild or moderate stage of Alzheimer's Disease, according to the National Institute of Neurological and Communicative Disorders and Stroke-Alzheimer's Disease and Related Disorders Association (NINCDS-ADRDA) criteria.
• MMSE score 16 to 26
• Physical clearance for study participation as evaluated by the clinician.
• Caregiver (spouse, family member, etc.) who agrees to and is capable of taking care and being responsible for the participation of the patient in the study (keeping a diary of health measures they collect on the patient at home, logging the patient's condition daily, and assuming responsibility for administering daily in-home treatment). Caregiver to have non-impaired mental abilities and normal motor skills, as determined by the investigators at screening. The definition of caregivers for this study is adults providing unpaid care to relatives or friends to help them take care of themselves in such activities as managing finances, shopping, preparing meals, and going to doctor appointments.
• Agreement to participate in approximately 10 weeks during the study.
• Normal to near-normal vision and hearing with correction as needed (e.g. corrective lenses, hearing aid).
• Fluent in English
• Minimum of 8th grade education
• Head circumference between 53 - 58 cm (to minimize variability in head antenna locations)
• If medicated for AD, then use of cholinesterase inhibitors and/or memantine for at least 3 months, on stable dose for at least 60 days prior to screening, and maintenance on that dose for the period of this study.
• All other non-AD medications must be stable for a period of 4 weeks prior to screening

Exclusion Criteria

• CDR Global Score of 0, 0.5 or 3
• Severe agitation
• Mental retardation
• Unstable medical condition
• Use of benzodiazepines or barbiturates 2 weeks prior to screening
• Participation in a clinical trial with any investigational agent within 6 months prior to study enrollment and no history of immunotherapy research participation
• History of Epileptic Seizures or Epilepsy
• Patients with major depression (not controlled with medication), bipolar disorder or psychotic disorders or any other neurological or psychiatric condition (whether now or in the past). The investigator will obtain this information from available patient medical records, history provided by the patient and caregiver, interview, and neurological exam.
• Alcoholism or drug addiction as defined by DSM-IV within last 5 years (addicted more than one year and or in remission less than 3 years) or severe sleep deprivation
• Patients with metal implants in the head, (i.e. cochlear implants, implanted brain stimulators, aneurysm clips) with the exception of metal implants in mouth
• Patients with vitamin B12 deficiency, abnormal thyroid function, or personal history of either any clinically defined medical disorder or any clinically defined neurological/psychiatric disorder (other than AD), including (but not limited to):, stroke, brain lesions, , cerebrovascular condition, other neurodegenerative disease, significant head trauma (loss of consciousness greater than half an hour, or related anterograde amnesia), multiple sclerosis; or personal history of previous neurosurgery or brain radiation
• Patients with any signs or symptoms of increased intracranial pressure, as determined in a neurological exam.
• Patients with demonstrated brain micro-hemorrhages at screening
• Patients with a score of 4 or higher on the Hachinski Test
• Patients with a score of 2 or less on the Global Deterioration Scale
• Patients with hypertension that is unresponsive to anti-hypertensive medications
• Patients with a history of migraine headaches occurring more than once a month
• Patients with a history of cancer within the last 3 years
• Patients chronically taking anticoagulants or anti-platelets (at discretion of Principal Investigator)
• Pregnant women and women who have the ability to become pregnant
• Patients with compressed hair thickness of more than 5mm (which could increase distance between head antennas and the scalp).
• Cardiac pacemakers
• Implanted medication pumps
• Intracardiac lines
• Significant heart disease

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
TEMT Treatment	MemorEM 1000	Patients in this arm will receive Transcranial Electromagnetic Treatment (TEMT) twice daily for a two-month treatment period utilizing the MemorEM 1000 head device.

Primary Outcome Measures

Name	Time	Method
ADAS-Cog	Change from baseline ADAS-Cog at 2 months	ADAS-Cog is the standard/benchmark test of cognitive performance evaluated in Alzheimer's-related clinical trials.

Secondary Outcome Measures

Name	Time	Method
Digit span score	Change from Baseline Digit span score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Diffusion Tensor Imaging (DTI)	Change from baseline DTI at 2 months	DTI is an MRI scan used to evaluate brain functional connectivity
Blood and CSF beta-amyloid levels	Change from Baseline beta-amyloid levels at 2 months	Blood and CSF will be analyzed for the toxic protein beta-amyloid
Blood and CSF tau levels	Change from Baseline tau levels at 2 months	Blood and CSF will be analyzed for the toxic protein tau
ADCS-ADL score	Change from Baseline ADCS-ADL score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Susceptibility-Weighted Imaging (SWI)	Change from Baseline SWI at 2 months	SWI is an MRI scan used to determine any brain microhemorrhages or tumors
Clock draw score	Change from Baseline Clock draw score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Blood and CSF markers of immune function	Change from Baseline pro- and anti-inflammatory cytokine levels at 2 months	Blood and CSF will be analyzed for pro- and anti-inflammatory cytokines (same measure units)
Blood and CSF markers of oxidative stress	Change from Baseline oxidative stress levels at 2 months	Blood and CSF will be analyzed for oxidative markers (same measure units)
MMSE score	Change from Baseline MMSE score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Global Deterioration score	Change from Baseline Global Deterioration score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Trails A & B score	Change from Baseline Trails A & B scores at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
Adverse Event Assessment	Change from Baseline Adverse Event Assessment at 2 months	AEA will be the primary safety outcome measure
Rey AVLT score	Change from Baseline Rey AVLT score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.
FDG-PET	Change from baseline FDG-PET at 2 months	FDG-PET scanning is used to determine brain energy metabolism/utilization
Resting state fMRI	Change from baseline rsfMRI at 2 months	rsfMRI is an MRI scan used to evaluate brain functional connectivity
Hachinski score	Change from Baseline Hachinski score at 2 months	This is a secondary cognitive outcome to assess effects of treatment on cognition.

Trial Locations

Locations (1)

Byrd Alzheimer's Institute, University of South Florida; 🇺🇸 Tampa, Florida, United States