Dual Field PEMF Therapy in Lower Extremity Painful Diabetic Distal Symmetric Peripheral Neuropathy

Not Applicable

Completed

• Conditions: Diabetic Neuropathy Peripheral
• Interventions: Device: Inactive (sham) Provant Therapy System; Device: Active Provant Therapy System

• Registration Number: NCT03455543
• Lead Sponsor: Regenesis Biomedical, Inc.

Brief Summary

Part A of this trial is a multi-center, prospective, double-blinded, sham-controlled, randomized clinical trial. Part A will evaluate PEMF treatment compared to sham treatment in patients with painful diabetic distal symmetric peripheral neuropathy (DSPN) when treatment is administered 30 minutes twice daily through a 120-day period (4 months). Part B is a 8-month open-label active treatment extension period designed to collect longer-term data on pain, medication use, quality of life and safety (Part B).Part B of this trial is a an extension period upon completion of Part A.

Detailed Description

Eligible subjects will be entered into a 14-day ePRO diary run-in period to collect average baseline pain scores related to their diabetic neuropathy in the lower extremities, diary compliance, and analgesic consumption (maintenance and prn prescribed peripheral neuropathic pain medication pill counts). Subjects will collect electronic patient-reported outcome (ePRO) data each morning around the same time during the run-in period.

Subjects will return to the clinic at Baseline (Day 0) for review of eligibility, diary compliance, average baseline diabetic neuropathic pain score of ≥4 and \<9, and review of stable analgesic pain consumption profile during the 14-day run-in period. Qualified subjects based on diary compliance and average pain score will be randomized 1:1 (active: sham) and will be instructed to self-treat twice daily for 120 days. Subjects will record electronic patient-reported outcome (ePRO) data following each morning treatment for 120 days. Subjects consenting to distal thigh and distal leg skin biopsies during the Screening visit will have biopsies collected and sent to the central laboratory for assessment. All subjects will have baseline assessments conducted.

Subjects will receive a telephone call at Day 7 to ensure compliance to treatment and diary completion, provide follow-up information on the biopsy sites (if applicable), complete a blinding assessment as well as be assessed for safety and concomitant medication changes.

At Month 1 subjects will return to the clinic for evaluation of safety, concomitant medication changes, review device usage and ePRO diary completion, and Patient Global Impression (PGI). Treatment satisfaction will also be assessed.

At Month 2 subjects will return to the clinic for evaluation of safety, concomitant medication changes, treatment satisfaction, review of device usage (reports will be supplied to the site) and ePRO diary completion, quality of life outcomes (WPAIQ and NeuroQoL), Patient Global Impression (PGI), and interim visit measurements of SPP.

At Month 3, subjects will return to the clinic for evaluation of safety, concomitant medication changes, review device usage (reports will be supplied to the site) and ePRO diary completion, and Patient Global Impression (PGI). Treatment satisfaction will also be assessed.

At Month 4 (end of Part A / start of Part B), subjects will return to the clinic for evaluation of safety, treatment satisfaction, review of device usage (reports will be supplied to the site), HbA1c, concomitant medication changes, weight, quality of life outcomes (WPAIQ and NeuroQoL), PGI, final measurements of SPP, NCS, QST and be assessed to determine their Toronto Clinical Neuropathy Score. Those subjects who consented and had biopsies collected at the Enrollment visit, will have their end of study biopsies during this visit and samples sent directly to the central laboratory for assessment. Subjects will return the study device and complete a blinding assessment.

Subjects that complete Part A will continue into the open-label extension period (Part B). All subjects will be reconsented if not completed at a prior visit and given an open-label active device. Subjects will record ePRO data for one week prior to the Month 6, 8, 10, and 12 visits following each morning treatment. Subjects will be reminded of the150-day (Month 5) phone call.

At Month 5, subjects will receive a telephone call to ensure compliance to treatment, and to be assessed for safety and concomitant medication changes.

At Month 6, subjects will receive a telephone call to ensure treatment compliance and collection of diary data, and to assess safety and concomitant medication changes.

At Month 7, subjects will receive a telephone call to ensure treatment compliance, and to assess safety and concomitant medication changes.

At Month 8, subjects will return to the clinic for evaluation of safety, measure QST, treatment satisfaction, review of device usage and collection of diary data, concomitant medication changes, quality of life outcomes (NeuroQoL), and PGI.

At Month 9, subjects will receive a telephone call to ensure treatment compliance, and to assess safety and concomitant medication changes.

At Month 10, subjects will receive a telephone call to ensure treatment compliance and collection of diary data, and to assess safety and concomitant medication changes.

At Month 11, subjects will receive a telephone call to ensure treatment compliance, and to assess safety and concomitant medication changes.

At Month 12 (end of open-label treatment extension), subjects will return to the clinic for evaluation of safety, weight, QST, NCS, TCNSS, PGI, treatment satisfaction, review of device usage and collection of diary data, concomitant medication changes, quality of life outcomes (NeuroQoL), and will return the study device. Subjects who consented and had biopsies collected at the 4 Month visit, will have their end of study biopsies performed during this visit.

Study Timeline

• Study First Submitted: 2018-02-28
• Study First Submitted QC: 2018-02-28
• Study First Posted: 2018-03-06
• Study Start: 2018-03-26
• Primary Completion: 2018-11-14
• Study Completion: 2019-07-18
• Results First Submitted: 2020-02-21
• Results First Submitted QC: 2020-02-21
• Results First Posted: 2020-03-09
• Status Verified: 2020-07
• Last Update Submitted: 2020-07-14
• Last Update Posted: 2020-07-15

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 182

Inclusion Criteria

• Type 1 or Type 2 diabetes
• Pain attributed to symmetrical lower extremity diabetic peripheral neuropathy for at least 6 months
• DPN pain over the preceding 24 hours is ≥4 and <9 based on the 11-point NPRS (0-10)
• 22 to 80 years of age
• On stable diabetes treatment
• HbA1c less than or equal to 10%
• No recent changes to analgesic prescriptions
• ABI of ≥0.8 to ≤1.3
• Walks independently
• Willing and able to give consent
• If female, must be post-menopausal, surgically sterile, abstinent or practicing an effective method of birth control
• Can access an internet browser or smart phone

To be randomized after the 14-day run-in period, average pain (NPRS) must be ≥ 4 and < 9 over preceding 7 days and subject must be 70% compliant with ePRO assessments (electronic diary)

Exclusion Criteria

• Active, open ulcer on either extremity
• Significant peripheral vascular disease
• Venous insufficiency
• History of solid organ transplant or severe renal disease
• Diagnosed with a non-diabetic cause of chronic neuropathy
• Previous or current history of primary or tertiary hyperparathyroidism, hypercalcemia, psychiatric disorder, alcohol dependency, Hepatitis B or C, or HIV infection
• Significant cardiovascular disease
• Uncontrolled medical illness
• Requires or anticipates the need for surgery during the study
• Total foot depth of >8 cm
• Has received any investigational drug or device within 30 days
• Has used systemic corticosteroids within 3 months
• History of malignancy within 5 years in treatment area
• A psychiatric disorder of sufficient severity
• Receiving prn narcotic medications
• History of drug or alcohol abuse within 1 year
• Implanted pacemaker, defibrillator, neurostimulator, spinal cord stimulator, bone stimulator, cochlear implant, or other implanted device with an implanted metal lead(s0
• Pregnant or planning to become pregnant
• Previous treatment with Provant Therapy
• Unwilling to follow instructions or comply with study instructions
• Pain from any other source that could confuse DPN pain assessment
• Clinically significant foot deformity
• Skin condition that could alter peripheral sensations
• Previous surgery to the spine or lower extremity with residual symptoms of pain or difficulty with movement.
• Clinically significant arthropathy

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Sham Group	Inactive (sham) Provant Therapy System	Treatment with in-active (sham) Provant Therapy System
Active Group	Active Provant Therapy System	Treatment with active Provant Therapy System

Primary Outcome Measures

Name	Time	Method
Change in Pain Intensity	Baseline through 4 months	Absolute change in pain intensity as measured by the 11-point, numerical pain rating scale (NPRS) (0-10; where 0=no pain, to 10=worst possible pain).

Secondary Outcome Measures

Name	Time	Method
Patient Global Impression at 4 Months	Baseline through 4 months.	Patient Global Impression at 4 Months. The question assesses change since the start of the study on a 7-point scale ("Since the start of the study, how has your diabetic neuropathy in your legs changed?"), and to score it as either very much worse, much worse, minimally worse, no change, minimally improved, much improved or very much improved.
Patients With 2 Point or 30% Reduction in Pain at 4 Months	Baseline to 4 months	Percentage of patients who have either a 2 point or 30% reduction in (pain) NPRS at 4 Months.; Absolute change in pain intensity as measured by the 11-point, numerical pain rating scale (NPRS) (0-10; where 0=no pain, to 10=worst possible pain).
Time to 30% or 2-point Reduction in NPRS, Whichever Comes First, Through 4 Months	Through 4 months	Absolute change in pain intensity as measured by the 11-point, numerical pain rating scale (NPRS) (0-10; where 0=no pain, to 10=worst possible pain). Number of participants achieving a 30% or 2-point reduction at or prior to weeks 1, 4, 8, 12 and 17 are displayed below.
Change in Neuropathy Related Quality of Life (NeuroQoL) Between Baseline and End of Treatment at 4 Months.	Baseline to 4 months	A validated set of health-related quality of life measures that are domain specific.Subjects will completed 6 domains: (1) Pain, (2) Lost/Reduced Feeling, (3) Diffuse Sensory Motor Symptoms, (4) Restrictions in Activities of Daily Living, (5) Disruptions in Social Relationships, and (6) Emotional Distress.The short forms were completed by the subject at the Enrollment Visit and end of study visit (Day 121). Each question in the domain was rated on a symptom scale from 1 (never) to 5 (all the time) and a bothersome scale from 1 (none) to 3 (very much).; The total score for the domain was calculated by multiplying the symptom score by the bothersome score. The scale range is from 1 to 15 where the minimum (best/least symptomatic) score is 1 and the maximum (worst/most symptomatic) score is 15. The mean change from Baseline to month 4 is displayed below.
Changes in Quantitative Sensory Testing (QST) Between Baseline and End of Treatment at 4 Months.	Baseline to 4 months	Contact thermal stimulation will be delivered using the Medoc Ltd. Q-Sense system to assess cool sensation threshold, warm sensation threshold and heat pain threshold modalities using the method of limits. Within the cool and warm sensation modalities, the trial is repeated 4 times on each foot and 3 times on each foot for heat pain threshold modality. The cool thermal testing will be conducted prior to the warm and heat pain thermal testing.; Mean change from baseline to 4-months displayed below.
Change is Skin Perfusion Pressure (SPP) for Baseline to End of Treatment at 4 Months	Baseline to 4 months	SPP was measured at two locations on each foot (dorsal right and left and plantar right and left). Mean change displayed from Baseline to 4-months displayed below.; SPP measures pressure in mmHg; an increase in pressure is favorable.; * Normal SPP: 50 mmHg to 100 mmHg; * Marginal Ischemia SPP: 30 mmHg to 50 mmHg; * Critical Limb Ischemia / PAD SPP: \< 30 mmHg
Changes in Nerve Conduction Studies of Velocity Between Baseline and End of Treatment at 4 Months.	Baseline to 4 Months	Using the NC-stat DPNCheck, the sural nerve conduction velocity was recorded on the right and left legs. An increase in velocity would suggest DPN improvement. The mean change from Baseline to 4-months is displayed below.
Changes in Nerve Conduction Studies of Amplitude Between Baseline and End of Treatment at 4 Months.	Baseline to 4 Months	Using the NC-stat DPNCheck, the sural nerve conduction amplitude was recorded on the right and left legs. An increase in amplitude would suggest DPN improvement. The mean change from Baseline to 4-months is displayed below.

Trial Locations

Locations (18)

Diabetes Research Center; 🇺🇸 Tustin, California, United States

River Birch Research Alliance, LLC; 🇺🇸 Blue Ridge, Georgia, United States

Wake Family Medicine, PC; 🇺🇸 Cary, North Carolina, United States

Mountain View Clinical Research; 🇺🇸 Denver, Colorado, United States

Heartland Research Associate, LLC; 🇺🇸 Wichita, Kansas, United States

Clinical Physiology Associates; 🇺🇸 Fort Myers, Florida, United States

Lake Internal Medicine Associates; 🇺🇸 Eustis, Florida, United States

Physician's Research Group; 🇺🇸 Mesa, Arizona, United States

Spotlight Research Center; 🇺🇸 Miami, Florida, United States

Clinical Research of Central Florida; 🇺🇸 Winter Haven, Florida, United States

Valley Clinical Research; 🇺🇸 Northridge, California, United States

Northern California Research; 🇺🇸 Sacramento, California, United States

MediSphere Medical Research Center, LLC; 🇺🇸 Evansville, Indiana, United States

Healthcare Research Network; 🇺🇸 Hazelwood, Missouri, United States

Palm Research Center; 🇺🇸 Las Vegas, Nevada, United States

The Center for Pharmaceutical Research, LLC; 🇺🇸 Kansas City, Missouri, United States

Great Lakes Medical Resarch; 🇺🇸 Westfield, New York, United States

Rainier Clinical Research; 🇺🇸 Renton, Washington, United States