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Rechargeable Neurostimulators in Deep Brain Stimulation for Psychiatric Disorders

Primary Purpose

Obsessive-compulsive Disorder, Depression

Status
Completed
Phase
Not Applicable
Locations
Study Type
Interventional
Intervention
Medtronic Restore Advanced 37713
Sponsored by
Universitaire Ziekenhuizen KU Leuven
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Obsessive-compulsive Disorder focused on measuring rechargeable neurostimulators

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • DBS for OCD / DBS for MD patients, AND
  • experiencing a beneficial effect of DBS on the psychiatric symptoms, AND
  • needing at least 1 IPG replacement per 18 months, AND
  • in the possibility to give informed consent for this study

Exclusion Criteria:

  • anyone not meeting all the inclusion criteria

Sites / Locations

    Arms of the Study

    Arm 1

    Arm Type

    Experimental

    Arm Label

    DBS for psychiatric disorders patients

    Arm Description

    Patients on deep brain stimulation for either obsessive-compulsive disorder or major depression, undergoing rechargeable neurostimulator implantation as intervention

    Outcomes

    Primary Outcome Measures

    Change in Y-BOCS (for OCD)
    Change in mean Yale-Brown Obsessive Compulsive Scale (Y-BOCS). Mean Y-BOCS during the first 2 years after intervention minus mean Y-BOCS during the last 2 years before intervention.
    Change in HAM-D (for MD)
    Change in Hamilton Depression Rating Scale (HAM-D). Mean HAM-D during the first 2 years after intervention minus mean HAM-D during the last 2 years before intervention.

    Secondary Outcome Measures

    Change in HAM-D (for OCD)
    Change in Hamilton Depression Rating Scale (HAM-D). Mean HAM-D during the first 2 years after intervention minus mean HAM-D during the last 2 years before intervention.
    Change in BDI
    Change in Beck Depression Inventory (BDI). Mean BDI during the first 2 years after intervention minus mean BDI during the last 2 years before intervention.
    Change in GAF
    Change in Global Assessment of Functioning (GAF). Mean GAF during the first 2 years after intervention minus mean GAF during the last 2 years before intervention.
    Change in Stimulation Amplitude
    Change in Stimulation amplitude as measured in volt. Mean stimulation amplitude during the first 2 years after intervention minus mean stimulation amplitude during the last 2 years before intervention.
    Change in Stimulation Frequency
    Change in Stimulation frequency as measured in hertz Mean stimulation frequency during the first 2 years after intervention minus mean stimulation frequency during the last 2 years before intervention
    Change in Pulse Width
    Stimulation pulse width as measured in seconds. Mean stimulation pulse width during the first 2 years after intervention minus mean stimulation pulse width during the last 2 years before intervention.
    Change in Contact Configuration
    Change in stimulation contact configuration as expressed in fraction of patients using a certain contact point as anode or cathode. Fraction of patients using a certain contact point as cathode or anode during the first 2 years after intervention minus fraction of patients using a certain contact point as cathode or anode during the last 2 years before intervention.
    Change in frequency of outpatient clinic contacts at the Psychiatry department
    Change in frequency of outpatient clinic contacts at the Psychiatry department. Frequency of outpatient clinic contacts at the Psychiatry department during the first 2 years after intervention minus frequency of outpatient clinic contacts at the Psychiatry department during the last 2 years before intervention.
    Change in fraction of hospitalized days at the Psychiatry department
    Change in fraction of hospitalized days at the Psychiatry department. Fraction of hospitalized days at the Psychiatry department during the first 2 years after intervention minus fraction of hospitalized days at the Psychiatry department during the last 2 years before intervention.
    Change in frequency of outpatient clinic contacts at the Neurosurgery department
    Change in frequency of outpatient clinic contacts at the Neurosurgery department. Frequency of outpatient clinic contacts at the Neurosurgery department during the first 2 years after intervention minus frequency of outpatient clinic contacts at the Neurosurgery department during the last 2 years before intervention.
    Change in fraction of hospitalized days at the Neurosurgery department
    Change in fraction of hospitalized days at the Neurosurgery department. Fraction of hospitalized days at the Neurosurgery department during the first 2 years after intervention minus fraction of hospitalized days at the Neurosurgery department during the last 2 years before intervention.
    Change in frequency of DBS-related surgical procedures
    Change in frequency of neurosurgical procedures related to the DBS system. Frequency of neurosurgical procedures related to the DBS system after intervention minus frequency of neurosurgical procedures related to the DBS system before intervention.
    Adverse events
    Adverse events

    Full Information

    First Posted
    February 3, 2016
    Last Updated
    February 17, 2016
    Sponsor
    Universitaire Ziekenhuizen KU Leuven
    Collaborators
    Medtronic
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    1. Study Identification

    Unique Protocol Identification Number
    NCT02685280
    Brief Title
    Rechargeable Neurostimulators in Deep Brain Stimulation for Psychiatric Disorders
    Official Title
    Feasibility Study Regarding the Implantation and Use of Rechargeable Neurostimulators in Deep Brain Stimulation for Psychiatric Disorders (Either Obsessive-compulsive Disorder or Major Depression)
    Study Type
    Interventional

    2. Study Status

    Record Verification Date
    February 2016
    Overall Recruitment Status
    Completed
    Study Start Date
    October 2007 (undefined)
    Primary Completion Date
    December 2014 (Actual)
    Study Completion Date
    December 2014 (Actual)

    3. Sponsor/Collaborators

    Responsible Party, by Official Title
    Sponsor
    Name of the Sponsor
    Universitaire Ziekenhuizen KU Leuven
    Collaborators
    Medtronic

    4. Oversight

    Data Monitoring Committee
    Yes

    5. Study Description

    Brief Summary
    From 1999 onwards, Deep Brain Stimulation [DBS] has been proposed as an alternative to capsulotomy in refractory cases of Obsessive-Compulsive Disorder [OCD]. More recently, several studies with DBS in patients with major depression have been initiated. In Belgium, there is currently a reimbursement for devices for DBS for OCD, but not for rechargeable neurostimulators, in these OCD patients. Although rechargeable neurostimulators are widely used in spinal cord stimulation for pain and DBS for movement disorders, they have not yet been used in DBS for psychiatric disorders population. Several possible problems might arise with the use of rechargeable neurostimulators in this highly specific population. In this prospective study with a before-after design, we would like to determine if the use of rechargeable neurostimulators is effective, applicable and safe and capable of diminishing the need for neurostimulator replacement procedures.
    Detailed Description
    BACKGROUND Obsessive-Compulsive Disorder [OCD] is a psychiatric disorder with a lifetime prevalence of 2% which is mainly characterized by obsessional ideas and compulsive behaviours and rituals. Many patients show improvement under cognitive behavioural and/or pharmacological treatment. A minority of patients is refractory to all available therapy and may benefit from capsulotomy1. From 1999 onwards, Deep Brain Stimulation [DBS] has been proposed as an alternative to capsulotomy in refractory cases of OCD (2,3). In Belgium, there is currently a reimbursement for devices for DBS for OCD, but not for rechargeable neurostimulators, in these OCD patients. STUDY RATIONALE Some patients with DBS for OCD need very frequent replacements of their neurostimulators (Medtronic Synergy 7427 ® [Synergy], Medtronic Kinetra 7428 ® [Kinetra] , Medtronic Activa PC 37601 ® [Activa PC] ), due to end-of-life of the batteries. This results in frequent re-interventions, probably causing discomfort for the patient, wound problems and infections due to revision surgery scar tissue, hardware problems and increasing costs for the public health system (consultations, hardware devices, surgery and its complications). A new type of neurostimulators with an externally rechargeable battery has been developed recently. The manufacturer estimates the longevity of these devices to be 9 years. These products are in conformity with the essential requirements of Directive 1999/5/EC on Radio and Telecommunications Terminal Equipment and Directive 90/385/EEC on Active Implantable Medical Devices. Currently they have a CE mark only for the indication of DBS for Parkinson's Disease and Essential Tremor, but not for DBS for psychiatric disorders such as OCD. Therefore, up till now they cannot be used in patients treated with DBS for OCD. Therefore, this physician-initiated study is trying to investigate whether the use of this new rechargeable neurostimulator is effective and safe in DBS treated OCD patients. HYPOTHESIS The hypothesis of the present study is that the implantation and use of rechargeable neurostimulators in OCD patients treated with DBS is (1) effective, (2) applicable, (3) safe and (4) decreases the need of neurostimulator replacement. OBJECTIVES To prove the hypothesis, the following objectives are aimed in our study: Efficacy: -To test whether DBS using rechargeable neurostimulators is effective on psychiatric symptoms as compared to DBS using non-rechargeable neurostimulators in these patients. Applicability: -To investigate whether this specific patient population is capable of recharging the rechargeable neurostimulators properly. Safety: -To document possible side effects of DBS for OCD using rechargeable neurostimulators. Capability of diminishing the need of neurostimulator replacement: -To investigate whether discomfort and risks of the frequent neurostimulator replacements due to battery end-of-life can be diminished by the use of the rechargeable neurostimulators. STUDY DESIGN At the Neurosurgery and Psychiatry consultation, eligible patients are informed about the present study. As soon as informed consent is obtained, the next time the battery of the non-rechargeable neurostimulator reaches its end-of-life and elective replacement is planned, a rechargeable neurostimulator and (if needed) the extension leads adaptors necessary to connect these neurostimulators with the existing extension leads will be implanted instead of a new non-rechargeable neurostimulator. After informed consent is obtained, at every consultation before and after implantation of the rechargeable neurostimulator the parameters as stated in the primary and secondary endpoints' sections will be recorded. TRIAL INTERVENTION The main trial intervention of this study will be the implantation of one rechargeable neurostimulator instead of the currently used non-rechargeable neurostimulator(s) and surgical closure of one of the existing abdominal wall cavities (the so-called "pockets"). It may be necessary to tunnel the extension cable from one side to another within the thoracic or abdominal wall. Thereby, we may provoke extension cable loops which may provoke undesirable stimulation when passing through a magnetic field. However this risk seems smaller than the risk of dissecting the electrode and replacing the extension cable to the other side. This intervention can be done under general or local anaesthetics. ADVERSE EVENTS REPORTING All adverse events are noted before and after implantation of the rechargeable neurostimulator. Below is a list of possible adverse events with both non-rechargeable and rechargeable neurostimulators for DBS in OCD: Early and late surgery and anaesthesia related problems A "pulling" experience at the level of the implanted neurostimulator and extension cables Postoperative pain and discomfort Displacement of the neurostimulator Erosion of the skin superficial to the implanted hardware Allergic reaction or rejection towards the implanted hardware Wound infection and infection of the implanted hardware Swelling or hematoma in the region of implantation Pain, itching or discomfort at incision/implant sites Death Hardware and directly stimulation-related problems Hardware failure (e.g. breakage or isolation damage of a cable, neurostimulator failure…) Unwanted spontaneous reset of the neurostimulator Fluctuating results Early end-of-life (less than expected) of the battery of the neurostimulator Playing with patient programmer Shocking or jolting stimulation Exceeding of the upper limit of current that is passed through the DBS system, as indicated by the manufacturer, that in extreme circumstances might lead to a biological effect at the tip of the electrode that is comparable to capsulotomy Electromagnetic interference might lead to dysfunction of the DBS system and in extreme circumstances even to death (e.g. during MRI scanning) Motor and movement problems Teeth grinding Akathisia Balance disturbance Coordination problems Torticollis Cheek twitches Other muscle contractions Increased tics Fractures Tremor Sleeping problems and fatigue Insomnia Hypersomnia Increased fatigue Vivid dreams and nightmares Gastro-intestinal problems Altered sensation of taste/smell Weight gain or weight loss Nausea and vomiting Increased hungriness or decreased appetite Esophagitis Slow gastric emptying Abdominal pain Diarrhoea or constipation Anal blood loss Mouth, ENT and respiratory problems Nose bleed Dental infections Dry mouth Tinnitus Hump of earwax Respiratory infection Shortness of breath Sleep apnoea Sexual and urinary problems Urinary, prostate or kidney infection Libido increase or decrease Erection decrease Ejaculation problem Vaginal discharge Urinary incontinence Increased urinary frequency Cardiovascular problems Palpitations Arterial hypertension Episodic retrosternal pain Neurologic problems Headaches A "flashing" sensation in the head Pain away from incision/implant sites Dizziness Sedation Paraesthesia Changes in handwriting Perseveration Seizures Coma Paralysis General problems Transpiration Warm and cold feeling Nail biting Body smell change Hair pulling Hair loss Skin and skin attachment infection Laboratory test abnormalities Increased creatine kinase Low ferritine Increased amylase Hypercholesterolemia Diabetes mellitus Psychiatric and cognitive problems Irritability Suicidality (thoughts/attempts) Increased depression Increased anxiety Increased OCD Aggression/violent behaviour Angry Overdrive Memory complaints Disinhibition Recklessness Hyperactivity Logorrhoea Accident proneness Hypomania Cognitive disturbance (clouding) Panic attack Tension/nervousness Hysteria Apathy Loss of motivation Lack of energy Flashbacks Confusion Blackouts Derealisation/depersonalisation Excessive alcohol drinking Medication abuse Paranoia Delusion Family problems Below is a list of possible adverse events with rechargeable but not with nonrechargeable neurostimulators for DBS in OCD: A heating sensation over the neurostimulator during recharging Local skin irritation over the neurostimulator during or after recharging Hardware failure of the recharger including breakage of the recharger fixation belt. Insufficient quality of the connection for energy transfer between the rechargeable neurostimulator and the recharger. The battery of the rechargeable stimulator always needs to be recharged before it is totally empty. After more than one episode of a totally empty battery further proper functioning of the neurostimulator nor replacement within the proposed study design cannot be guaranteed by the constructor. A committee consisting of the principle investigators will decide whether an adverse event is definitely, probably, possibly or not an adverse event due to the system for DBS for OCD. All expected and unexpected adverse events will be noted and published. BIOSTATISTICS AND DATA ANALYSIS Paired statistical tests for continuous data (A, f, PW, number of consultations,) and for ordinal data (Y-BOCS, GAF, HAM-A, HAM-D, BDI) pre- and post-implantation, as well as descriptive statistics for continuous data (number of recharging sessions, number of battery status controls, battery longevity, preferred stimulator type at replacement), will be used. No power calculation is performed. ETHICS Approval of the UZ/KU Leuven Ethics Committee, working after the ICH-GCP principles, will be asked for. All data will be collected in an objective, careful and precise manner. All risks will be kept as low as possible with a meticulous implantation procedure and a careful clinical evaluation before and after implantation. Participation in the study is completely voluntary.

    6. Conditions and Keywords

    Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
    Obsessive-compulsive Disorder, Depression
    Keywords
    rechargeable neurostimulators

    7. Study Design

    Primary Purpose
    Treatment
    Study Phase
    Not Applicable
    Interventional Study Model
    Single Group Assignment
    Masking
    None (Open Label)
    Allocation
    N/A
    Enrollment
    12 (Actual)

    8. Arms, Groups, and Interventions

    Arm Title
    DBS for psychiatric disorders patients
    Arm Type
    Experimental
    Arm Description
    Patients on deep brain stimulation for either obsessive-compulsive disorder or major depression, undergoing rechargeable neurostimulator implantation as intervention
    Intervention Type
    Device
    Intervention Name(s)
    Medtronic Restore Advanced 37713
    Other Intervention Name(s)
    Medtronic Restore 37711, Medtronic Activa RC 37612
    Intervention Description
    Rechargeable neurostimulators are implanted when the non-rechargeable neurostimulators are end-of-life.
    Primary Outcome Measure Information:
    Title
    Change in Y-BOCS (for OCD)
    Description
    Change in mean Yale-Brown Obsessive Compulsive Scale (Y-BOCS). Mean Y-BOCS during the first 2 years after intervention minus mean Y-BOCS during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in HAM-D (for MD)
    Description
    Change in Hamilton Depression Rating Scale (HAM-D). Mean HAM-D during the first 2 years after intervention minus mean HAM-D during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Secondary Outcome Measure Information:
    Title
    Change in HAM-D (for OCD)
    Description
    Change in Hamilton Depression Rating Scale (HAM-D). Mean HAM-D during the first 2 years after intervention minus mean HAM-D during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in BDI
    Description
    Change in Beck Depression Inventory (BDI). Mean BDI during the first 2 years after intervention minus mean BDI during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in GAF
    Description
    Change in Global Assessment of Functioning (GAF). Mean GAF during the first 2 years after intervention minus mean GAF during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in Stimulation Amplitude
    Description
    Change in Stimulation amplitude as measured in volt. Mean stimulation amplitude during the first 2 years after intervention minus mean stimulation amplitude during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in Stimulation Frequency
    Description
    Change in Stimulation frequency as measured in hertz Mean stimulation frequency during the first 2 years after intervention minus mean stimulation frequency during the last 2 years before intervention
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in Pulse Width
    Description
    Stimulation pulse width as measured in seconds. Mean stimulation pulse width during the first 2 years after intervention minus mean stimulation pulse width during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in Contact Configuration
    Description
    Change in stimulation contact configuration as expressed in fraction of patients using a certain contact point as anode or cathode. Fraction of patients using a certain contact point as cathode or anode during the first 2 years after intervention minus fraction of patients using a certain contact point as cathode or anode during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in frequency of outpatient clinic contacts at the Psychiatry department
    Description
    Change in frequency of outpatient clinic contacts at the Psychiatry department. Frequency of outpatient clinic contacts at the Psychiatry department during the first 2 years after intervention minus frequency of outpatient clinic contacts at the Psychiatry department during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in fraction of hospitalized days at the Psychiatry department
    Description
    Change in fraction of hospitalized days at the Psychiatry department. Fraction of hospitalized days at the Psychiatry department during the first 2 years after intervention minus fraction of hospitalized days at the Psychiatry department during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in frequency of outpatient clinic contacts at the Neurosurgery department
    Description
    Change in frequency of outpatient clinic contacts at the Neurosurgery department. Frequency of outpatient clinic contacts at the Neurosurgery department during the first 2 years after intervention minus frequency of outpatient clinic contacts at the Neurosurgery department during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in fraction of hospitalized days at the Neurosurgery department
    Description
    Change in fraction of hospitalized days at the Neurosurgery department. Fraction of hospitalized days at the Neurosurgery department during the first 2 years after intervention minus fraction of hospitalized days at the Neurosurgery department during the last 2 years before intervention.
    Time Frame
    from 2 years before intervention until 2 years after intervention
    Title
    Change in frequency of DBS-related surgical procedures
    Description
    Change in frequency of neurosurgical procedures related to the DBS system. Frequency of neurosurgical procedures related to the DBS system after intervention minus frequency of neurosurgical procedures related to the DBS system before intervention.
    Time Frame
    from initial electrode implantation through study completion (on average approximately 5 years)
    Title
    Adverse events
    Description
    Adverse events
    Time Frame
    from initial electrode implantation through study completion (on average approximately 5 years)

    10. Eligibility

    Sex
    All
    Minimum Age & Unit of Time
    18 Years
    Accepts Healthy Volunteers
    No
    Eligibility Criteria
    Inclusion Criteria: DBS for OCD / DBS for MD patients, AND experiencing a beneficial effect of DBS on the psychiatric symptoms, AND needing at least 1 IPG replacement per 18 months, AND in the possibility to give informed consent for this study Exclusion Criteria: anyone not meeting all the inclusion criteria
    Overall Study Officials:
    First Name & Middle Initial & Last Name & Degree
    Bart Nuttin, MD, PhD
    Organizational Affiliation
    Universitaire Ziekenhuizen KU Leuven
    Official's Role
    Principal Investigator

    12. IPD Sharing Statement

    Plan to Share IPD
    No

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