Clinical Trial Details
— Status: Completed
Administrative data
NCT number |
NCT01653340 |
Other study ID # |
CE100112 |
Secondary ID |
2012-002005-22 |
Status |
Completed |
Phase |
N/A
|
First received |
July 24, 2012 |
Last updated |
February 17, 2014 |
Start date |
May 2012 |
Est. completion date |
February 2014 |
Study information
Verified date |
February 2014 |
Source |
University of Roma La Sapienza |
Contact |
n/a |
Is FDA regulated |
No |
Health authority |
|
Study type |
Interventional
|
Clinical Trial Summary
The purpose of this study is to assess short- and long-term safety, tolerability and efficacy
of cervical High Frequency Spinal Cord Stimulation (HF-SCS) in patients suffering from
chronic migraine refractory to conventional medical therapy.
Description:
1. Introduction 1.1 Background Migraine is a common disabling headache disorder. Patients
with Chronic Migraine (CM) experience headache on a minimum of 15 days per month. CM is
associated with significant disability and reduced quality of life .
Since the late 1990s, there has been considerable progress in neurostimulation
techniques to treat medically intractable chronic-headache syndromes patients, by
applying peripheral-nerve stimulation to patients . It is indeed well demonstrated that
a non-painful stimulation of peripheral nerves can elicit analgesic effects, and that
occipital nerve stimulation (ONS), by retrograde activation of the trigemino-cervical
complex can provide effective pain relief in patients with headache disorders, including
migraine. Recently, high cervical spinal cord stimulation (SCS) has been tested for the
treatment of chronic cluster headache , highlighting a potential benefit of SCS over
ONS: SCS exerts an immediate and almost maximal effect, which allows a test phase prior
to implantation of the pulse generator with the possibility of removing the electrode in
case of insufficient pain relief.
Both SCS and ONS produce paresthesia, an unpleasant tingling sensation for the patients
In recent prospective studies, a new modality of SCS, High Frequency (HF) SCS, has been
demonstrated to be effective and safe in a chronic pain population, the Failed Back
Surgery Syndrome (FBSS) population . High Frequency SCS differs from conventional SCS in
several ways, which present significant advantages to both the patients and the
healthcare professionals: 1) absence of paresthesia (tingling) which leads to greater
patient comfort and acceptance of the therapy, 2) shorter procedural time as no
paresthesia mapping is needed, and 3) increased efficacy compared to conventional SCS,
demonstrated in the FBSS population. Additionally, HF SCS has a similar safety profile
as conventional SCS.
HF-SCS may thus combine the advantage of paresthesia free therapy (and thus greater
patient tolerability of the therapy) with the possibility of testing the therapy during
a trial phase prior to the implantation of a permanent pulse generator.
2. Study Objective, Outcomes, and Design 2.1 Objective The objective of this study is to
investigate the safety, efficacy and tolerability of high frequency (HF) Spinal cord
stimulation (SCS) for the treatment of patients with chronic migraine.
2.2 Outcomes
- Change of frequency in headache days from baseline;
- Change of frequency in migraine days from baseline;
- Change in frequency of moderate/severe headache days from baseline;
- Change in headache pain Visual Analog Scale (VAS) score from baseline;
- Change in HIT-6 score from baseline;
- Change in Migraine Disability Assessment (MIDAS) Score from baseline;
- Change in frequency of triptans intake from baseline;
- Patient Global Impression of Change (PGIC);
- Change in Quality of Life from baseline;
- Change in the number of sleep disturbances per night from baseline;
- Incidence of device-related adverse events.
2.3 Target Size This feasibility study will enroll a minimum of 10 subjects and a
maximum of 20 subjects.
Each subject will undergo a trial phase of the therapy. If the trial is successful, the
subjects will be followed-up for 6 months, with regular clinic follow-up visits.
It is expected that the first subject will be enrolled in June 2012. The last subject is
expected to complete the study follow-up period by January 2013.
2.4 Devices Used
The Senza™ System, manufacturer by Nevro (Menlo Park, USA), received CE mark in 2010 for
use as an aid in the management of chronic intractable pain of the lower trunk and/or
limbs. The Senza System is similar to other available SCS systems in design and
function. However, Nevro's proprietary waveform algorithms may eliminate unwanted side
effects, improve subject experience and potentially provide better pain relief.
Similar to the commercial systems, the Senza System includes lead(s), anchor(s),
extension(s), trial stimulator, implantable pulse generator (IPG), charger, patient
remote control, and clinician programmer. Additional components include surgical tools,
cables and various other accessories for use in the placement of the leads and IPG.
3. Selection and Withdrawal of Subjects
This study will recruit subjects with chronic headache migraine as per the International
Classification of Headache Disorders (2nd edition) .
3.1 Inclusion/Exclusion Criteria
To participate in the study, the subject must meet all of the following criteria:
Include a subject who has (is):
- An adult between the age of 18 and 65
- Capable of providing informed consent
- A diagnosis of chronic (>15 or more headache-days per 4 week period for more than 3
months, with an headache-day being defined as a day with an attack lasting a
minimum of 4 hours) migraine refractory to conventional medical treatment (has
failed at least 2 preventive and 2 abortive drugs) as per the ICHD-II guidelines.
- On optimal and stable preventive headache pharmacological migraine therapy for at
least 2 months
- Failed treatment with Onabotulinumtoxin A for 12 months
- Able to comply with the requirements of the study visits and self-assessment
questionnaires Able to provide informed consent and willing to comply with study
procedures
Exclude a subject who has (is):
- medication-overuse headache
- Had treatment with Onabotulinumtoxin A in the last 3 months
- An already implanted active medical device
- A contraindication to the cervical placement of SCS lead
- A life expectancy of less than 1 year
- A female of child bearing potential who is pregnant/lactating or not using adequate
birth control
- Beck Depression Inventory score of >24
- Evidence of an active disruptive psychological/psychiatric disorder or other known
condition significant enough to impact perception of pain (e.g. fibromyalgia),
compliance of intervention and/or ability to evaluate treatment outcome as
determined by the Investigator
- Addiction to any of the following: illicit drugs, alcohol (5 or more drinks/day),
and/or medication
- Bleeding diathesis such as coagulopathy or thrombocytopenia
- Immuno-compromised and at risk for infection
- Diabetic which is not under control as determined by the Investigator
- Unresolved issue of secondary gain
- Inability to manage the technical demands of the SCS equipment
- Currently participating in a randomized clinical trial with an active treatment arm
or planned to be enrolled in another clinical trial 3.2 Subject Early Withdrawal
A subject may be withdrawn early from the study for the following reasons:
- Adverse event
- Non-compliance
- At the discretion of the Investigator
- Subject withdrawal of consent
- Study is stopped by the Investigator or Ethics Committee (EC) 3.3 Device
Explantation At the discretion of the Investigator or subject, the IPG and/or the
leads(s) may be explanted from a subject. If the explantation is as a result of an
unanticipated adverse device effect (UADE) or device failure, the Investigator will
send the explanted devices and accessories (i.e., Remote Control) to Nevro for
device analysis.
If the subject is experiencing an adverse event related to the explant, the subject will
be followed until resolution of that adverse event or determination that the subject's
condition is stable. The Investigators or the EC may suspend or terminate the study
early at any time. If the study is suspended or terminated prematurely, all currently
enrolled subjects will be withdrawn from the study.
4. Treatment of Subjects/Study Procedures 4.1 Screening/enrollment The Investigator will
identify potential study candidates who are likely to meet study inclusion and exclusion
criteria and discuss participation in the study. If the subject agrees, the Investigator
and research staff will meet with the subject to review details of the study. The
subject will have the opportunity to read the informed consent and ask any questions.
This study is entirely voluntary. Subject consent will be obtained in accordance and in
compliance with Good Clinical Practice guidelines and Italian regulations.
If the subject agrees to participate in the trial he/she will sign the consent form.
After the subject provides informed consent, he/she is considered enrolled into the
study.
The subject will be asked to attend the clinic to complete a series of subject
questionnaires to gather information on their condition and current level of pain,
disability and affected lifestyle metrics.
Enrolled subjects will undergo a 2 week HF-SCS trial. 4.2 Trial Phase During the trial
implant, the 2 leads will be positioned to cover the C2-C3 cervical levels.
Over the following 2 weeks, the investigator will optimize therapy delivery by
identifying the stimulation settings providing maximal headache pain relief.
During this period, the patient will complete daily a headache diary to record their
headache frequency, intensity and duration.
The subject will be asked to attend the clinic at the end of the trial period. Together
with his/her physician, the subject will discuss his/her experience over the past 2
weeks (satisfaction with the therapy), and decide whether or not move forward with a
Nevro Senza™ IPG. If the subject chooses not to move ahead, she/he will be given
alternative treatment options by the physician, and no further follow up study
procedures will be required.
During the trial phase, and until the 3 month follow-up visit, the physician will try to
keep the headache medication as stable as possible, in order to avoid confounding
factors when investigating the efficacy of the therapy Permanent Implant The Nevro
Senza™ IPG will be implanted in the buttock or abdomen area as outlined in the
Physician's Manual. Fluoroscopy and impedance measurements may be used during the
procedure to confirm lead placement and location.
As per the Investigator's standard clinical practice the subject will be placed on
prophylactic antibiotics as a preventative for skin flora (bacteria) infections.
Subjects will follow the Investigator's protocol for anticoagulant therapy and other
medications.
Before hospital discharge, the IPG will be programmed with the optimal settings
identified during the trial phase. The Patient Manual will be reviewed with the subject
and a copy will be given to the subject for future reference 4.3 Follow-Up Visits
Subjects implanted with an IPG will be asked to attend in-clinic visits at 3 and 6
months post IPG implantation.
During these visits, the subjects will undergo a clinical assessment and the following
data will be collected on Case Report Forms (CRFs):
- Medication usage
- Headache Impact Test (HIT)-6 questionnaire
- Migraine Disability Assessment (MIDAS) questionnaire
- Quality of Life questionnaire
- Patient Global Impression of Change (PGIC) scale
- Patient Sleep disturbances
The patient headache diary will be reviewed and a new one provided for the next
follow-up period.
During these visits, all Adverse Events will be documented. Until the 3 month follow-up
visit, the physician will try to keep the headache medication as stable as possible, in
order to avoid confounding factors when investigating the efficacy of the therapy
At the end of the 6-months period, the study will be completed and the subjects will
continue to be followed-up as per the center standard practice.
4.4 Interim/Unscheduled Visits Subjects may be seen in the clinic for
interim/unscheduled visits at any time during study. Possible reasons for an
interim/unscheduled visit include the need to modify device programming to adjust pain
relief, or for an adverse event. Such visits will be documented on CRFs.
5. Data Measures and Analysis Both qualitative and quantitative data will be collected and
analysed. Table 1: Data Collection per visit
CRFs Enrollment Trial implant End of trial IPG implant Month 3 Month 6 Enrollment x
Medical history x Medication usage x x x x Questionnaires (HIT-6, MIDAS, QoL, PGIC) x x
x x Implant details x x Patient diary x x x x x Adverse Event x x x x x
General descriptive measures will include counts and percentages for categorical
measures and the mean, standard deviation, median, and minimum and maximum values for
continuous data.
Non-parametric 2-tailed cross sectional and pair-wise comparisons will be undertaken.
Simple linear and non-linear regression will be used to calculate predictor values from
the vertebral level data collected. Significance will be set at the 0.05 level.
Additional analyses may be conducted.
6. Adverse Events 6.1 Definitions The definitions presented in this section allow for a
clear understanding of adverse event data collection and reporting requirements.
6.1.1 Adverse event An adverse event (AE) is defined as any undesirable clinical
occurrence in a subject that appears or worsens in the clinical study (as compared to
the subject's baseline health) and is any untoward medical occurrence defined as an
unintended disease or injury or untoward clinical signs (including abnormal laboratory
findings) in a subject whether or not related to the investigational or commercial
medical device. This definition includes events related to the study medical devices and
events related to the study procedures. An AE is also any event related to any
underlying medical condition, present at baseline, which increases in severity by a
clinically meaningful amount during the study as determined by the Investigator.
Adverse events will be summarized by type, severity, treatment/intervention provided,
relationship to the device/procedure, and resolution.
As the primary efficacy measure in this study is pain, back and leg pain does not need
to be reported as an adverse event unless it meets the definition of a serious adverse
event. However, Investigators may, at their discretion, report any pain-related adverse
events during the study.
Pre-existing conditions will not be reported as an adverse event unless there has been a
substantial increase in the severity or frequency of the problem which has not been
attributed to natural history.
6.1.2 Serious adverse events
A serious adverse event is an adverse event that:
- Leads to death
- Leads to a serious deterioration in the health of the subject that:
- Results in life-threatening illness or injury
- Results in a permanent impairment of a body structure or a body function
- Requires in-subject hospitalization or prolongation of existing hospitalization
- Results in medical or surgical intervention to prevent permanent impairment to body
structure or a body function
- Leads to fetal distress, fetal death, or a congenital abnormality or birth defect
6.1.3 Adverse device effect
An adverse device effect (also called a device-related adverse event) is an adverse
event with a reasonable possibility that the device caused or contributed to the event.
During this clinical investigation an event should be considered related to the device
when it is the result of:
- The device components (e.g., lead, extension, IPG)
- The implant procedure
- The therapy/stimulation 6.1.4 Serious adverse device effect An untoward medical
occurrence that happens in a subject, is related to the investigational device,
procedure, or therapy and is serious, but is not unanticipated is a serious adverse
device effect (SADE). Untoward medical occurrences that are anticipated, i.e. are
unsurprising, are identified in the investigator's brochure or protocol and
informed consent form.
Anticipated adverse events related to the device, procedure or therapy are listed in
section 7, Risk/Benefit.
6.1.5 Unanticipated serious adverse device effect An untoward medical occurrence that
happens in a subject, is related to the investigational device, device procedure, or
therapy, is serious, and is unanticipated is classified as an unanticipated serious
adverse device effect (USADE).
Anticipated adverse events related to the device, procedure or therapy are listed in
Section 7, Risk/Benefit.
6.1.6 Severity
The Investigator will use the following definitions to rate the severity of each adverse
event:
- Mild: Awareness of a sign or symptom that does not interfere with the subject's
usual activity or is transient, resolved without treatment and no sequelae
- Moderate: Interferes with the subject's usual activity or requires symptomatic
treatment
- Severe: Symptom(s) causing severe discomfort with significant impact of the
subject's usual activity and requires treatment 6.2 Reporting The Investigator will
assess the subject for adverse events and capture the required adverse event
information in the subject records or an appropriate study form. Adverse events can
be based on subject report. Subjects should be instructed to contact their
physician in the case of emergency, as described in the informed consent.
All AEs will be followed until the event is resolved (with or without sequelae). If an
event is ongoing at the time study completion of termination, the subject will be
followed until resolution or Investigator determination that the subject's condition is
stable.
The Investigator is responsible for reporting information regarding specific AEs (e.g.
SAEs and UADEs) to the appropriate EC as required by local regulations. The Investigator
will also report any UADEs and appropriate device related AEs to Nevro.
7. Risk/Benefit 7.1 Potential Risks A risk analysis was completed by Nevro Corporation in
accordance with ISO 14971 - Application of Risk Management for Medical Devices. This
analysis showed that the Senza System exhibits a safety profile equivalent to the
commercially available stimulators.
In an effort to report all of the potential risks for this study, all adverse events
attributed to the device, procedure or stimulation therapy reported in a review of key
SCS literature (Cameron 2004; Kumar et al. 2007) are described in this section. Table 2
lists the adverse events that were reported in these articles in order of frequency
reported in the Cameron article. These are foreseeable risks that are presented in the
informed consent and are typical of commercial SCS systems.
Other adverse events which may potentially occur, but were not reported in the Cameron
and Kumar articles, include: increased intensity, duration, or frequency or back and/or
leg pain, uncomfortable stimulation of tissue around the leads including skin and
muscle, development of pain symptoms in a new location, thrombosis, nerve injury,
seizure, and death.
As the primary efficacy measure in this study is pain, headache pain does not need to be
reported as an adverse event unless it meets the definition of a serious adverse event.
However, Investigators may, at their discretion, report any pain-related adverse events.
Table 2: Risks Associated with Spinal Cord Stimulation Cameron 2004 Kumar 2007 n =
2107-2972
% n = 84
% Lead migration 13.2 9.5 Lead breakage 9.1 2.4b Infection 3.4 8.3a Hardware malfunction
2.9 nr Unwanted stimulation 2.4 1.2c Battery failure 1.6 nr Other 1.4 nr Pain over
implant 0.9 6.0 Loose connection 0.4 1.2 CSF leak 0.3 1.2d Hematoma 0.3 nr Skin erosion
0.2 nr Allergic reaction 0.1 nr Paralysis 0.03 nr Neurostimulator pocket fluid
collection/seroma 0.0 4.8 Intermittent stimulation 0.0 nr Epidural hemorrhage 0.0 nr
Loss of therapeutic effect, loss of paresthesia, or unpleasant paresthesia nr 7.1
Techniquee nr 2.4 IPG migration nr 1.2 Abbreviations: nr, not reported. a reported as
"infection and wound breakdown" b reported as "lead extension fracture/torqued contacts"
c reported as "anteriorly placed electrode caused shocks" d reported as "dural tear" e
cap not installed on IPG when only one lead was implanted (1), lead cut during implant
(1)
7.2 Possible Benefits The Senza System has received CE mark approval for use in the
treatment of chronic intractable pain. The hazards and mitigation mechanisms were
identified and risk factors were calculated for each of the identified hazards and were
found to be within the acceptance criterion. The results of the risk analysis concluded
that the benefit of providing pain relief for subjects suffering from chronic
intractable pain outweighs the residual risks that may be posed by the use of this
device.
The desired benefit is the improvement in the status of the patient's refractory pain.
There is however, no guarantee that this will happen. Results of prior and on-going
clinical studies show that the Senza System offers an opportunity for improved pain
relief in this chronic intractable pain population. Thus, by participating in this study
the information gathered will add to the understanding of treatment options for patients
with chronic migraine. This knowledge may advance medical science and may benefit other
patients with chronic pain and potentially society at large.
8. Conduct of Study
8.1 Statement of Study Compliance The study will be performed in accordance with ISO
14155-2011, Good Clinical Practice (GCP) guidelines, recommendations guiding physicians
in biomedical research involving humans adopted by the 18th World Medical Assembly,
Helsinki, Finland (1964 and later revisions). The Investigator, as required by the local
regulations should notify the EC in writing after completion, termination, or
discontinuation of the study at the site. If study is discontinued due to safety
concerns, the Investigator will notify the EC immediately.
8.2 Investigator Responsibilities The Investigator is responsible for ensuring that the
investigation is conducted according to the study protocol, and applicable ISO EN
14155-2011, data protection regulations, and any other applicable Ethics Committee=
requirements.
The Investigator(s) shall be responsible for the day-to-day conduct of the investigation
as well as for the safety and well-being of the human patients involved in the clinical
investigation.
It is the responsibility of the Investigator to obtain approval of the study protocol
from the EC and to keep the EC informed of any serious adverse events, unanticipated
adverse device effects, and amendments to the protocol. All correspondence with the EC
should be filed by the Investigator.
8.3 Quality Control and Quality Assurance All documents and data shall be produced and
maintained in such a way to assure control of documents and data to protect the
patient's privacy as far as reasonably practicable. Representatives of the applicable
regulatory authorities are permitted to inspect the study documents (e.g., study
protocol, CRFs, and original study-relevant medical records/files) as needed. All
attempts will be made to preserve patient confidentiality.
8.4 Ethics The Investigator is a physician whose first responsibility is to the care of
the patient. Should individual care conflict with study requirements, it is understood
that the care of the patient is foremost. In all respects, this study shall be conducted
pursuant to the "Declaration of Helsinki: Recommendations Guiding Medical Doctors in
Biomedical Research Involving Human Subjects".
At all times, the Investigators are to follow this confirmatory study plan, abide by all
Good Clinical Practice requirements set by prevailing national law and any EC
regulations.
8.5 Termination or Suspension of the Investigation The study may be terminated when all
of the requirements of the protocol have been fulfilled. Patients will be considered to
have completed all study requirements following completion of the 6 month visit.
The Investigators or EC may suspend or terminate the study early at any time. If the
study is suspended or terminated prematurely, all currently enrolled patients will be
withdrawn from the study. If there is an ongoing event related to the device or therapy,
the patient will be followed until resolution of that adverse event or determination
that the subject's condition is stable.
9. Data Handling and Recordkeeping
All documents will be maintained by the Investigator. The data will be collected using
appropriate questionnaires and will be secured by the Investigator. The Investigator will be
required to keep study records as dictated by local regulations.
Appendix A - Responsibilities of Investigators
The Investigator is responsible for ensuring that this clinical study is conducted according
to all conditions of the HREC approval and applicable regulations. The Investigator is
responsible for ensuring that informed consent is obtained from all subjects prior to any
diagnostic tests or treatments that are outside the standard course of treatment that would
be followed if this subject were not being considered for enrollment in this clinical study.
Subjects will be informed that they are free to refuse to participate in this clinical study
without loss of benefits to which they are otherwise entitled, and that if they choose to
participate, they may withdraw at any time without prejudice to future care. The informed
consent approved by the HREC must be signed prior to study participation. The original signed
informed consent for each subject must be retained by the Sponsor Investigator.
Other specific responsibilities of the Sponsor Investigator include:
Awaiting Approval The Investigator may discuss with a subject their interest in participating
in the clinical study, but shall not request the written informed consent nor allow any
subject to participate in the clinical study before HREC and other necessary approvals are
received.
Subject records Subject records include signed informed consent forms, copies of all
completed case report forms and supporting documents (laboratory reports, reports of
diagnostic tests, medical records, etc.) and records of exposure of each subject to the
device. Informed consent must comply with EN/ISO 14155-2011.
Documentation of the Use of the Device without Informed Consent The Investigator must
document use of the device without Informed Consent. The Investigator is responsible for
reporting device usage without prior informed consent per the applicable regulations.
Unanticipated Adverse Device Effects The Investigator is responsible for maintaining records
of all reports and information pertaining to unanticipated adverse device effects.
Ethics Committee Information The Investigator is responsible for maintaining all information
pertaining to EC review and approval of this clinical study including a copy of the EC letter
approving the clinical study, a blank informed consent form approved by the EC and that the
EC approved the protocol.