PTSD Clinical Trial
Official title:
Xyrem for Treatment Refractory Insomnia Due to PTSD
Xyrem (sodium oxybate) is an agent with the propensity to improve slow wave sleep and sleep
efficiency. It is FDA approved to treat cataplexy (drop attacks) associated with narcolepsy
(sleep attacks). It has been shown to be a safe and effective agent here where deep,
restorative slow wave sleep improves and next day cataplexy attacks tend not to occur.
Post Traumatic Stress Disorder (PTSD) is a psychiatric illness where a patient has witnessed
or been involved in a traumatic event. After the event is over, nightmares, flashbacks,
avoidance of people and places associated with trauma and hyperarousal occur which is
incapacitating to the patient. One major part of PTSD hyperarousal is marked insomnia with
multiple awakenings at night. This resultant poor sleep is compounded by use of SSRI
serotonergic antianxiety agents (ie Zoloft(sertraline)) as first line therapy which tend to
degrade slow wave, restorative sleep. Patients may respond to SSRI treatment but may fail to
remit as they continue to have sleep problems. PTSD patients will often fail to respond to
antihistamine (Desyrel (trazodone)) and benzodiazepine GABA hypnotic agents
(Restoril(temazepam)) and continue with poor, interrupted sleep. It is possible that Xyrem's
ability to remarkably improve slow wave sleep may greatly help treatment refractory insomnia
due to PTSD.
The author proposes an open-label study (no placebo) where 10 PTSD patients, who have failed
usual PTSD treatments and have failed usual insomnia treatments in particular will be given
Xyrem in addition to their current PTSD medication. The authors wish to determine if Xyrem
is a safe treatment optionin this difficult-to-treat patient population.
This is an open-label (no placebo) study to see if the addition of Xyrem to a subject's PTSD
medication regimen will be tolerated and possibly improve insomnia. Subjects will currently
be taking at least a single psychotropic agent for the treatment of PTSD, (an SSRI). Dosing
will be stable for at least 4 weeks and subjects will need to report continued insomnia
despite treatment. They must also have failed at least two insomnia augmentations from
separate drugs classes (benzodiazepine (temezapam, zolpidem, ect.), antihistime (quetiapine,
mirtazapine, trazadone, etc.), dopamine antagonist (olanzapine, quetiapine, aripiprazole,
etc.) to qualify for refractory insomnia.
Subjects will complete consenting process and attend a screening visit where they will be
given a MINI psychiatric diagnostic evaluation to confirm PTSD, be given a Hamilton Anxiety,
a Hospital Anxiety & Depression Scale, PCL-C, Fatigue Severity Scale, Epworth Sleepiness
Scale, Pittsburgh Sleep Quality Inventory, SF-12, and sleep diary evaluation to delineate
current anxiety levels (secondary measure). Subjects will have to offer consent for the
study team to contact their primary providers and retrieve all past and present records to
show refractory history and lack of substance abuse. Subjects will undergo a brief physical
exam and bloodwork and a sleep EEG will be ordered. Furthermore, a urine drug screen will be
used to screen for current misuse. If subjects are taking sleeping agents, they will be
appropriately washed out (tapered per cusual clinical practice and then drug free 5 times
the drug's half life) prior to sleep EEG and prior to Xyrem start. In clinical practice,
Xyrem use does not warrant blood monitoring, EEGs or EKGs per the FDA.
Assuming subject meets eligibility, they will start Xyrem per cataplexy dosing guidelines.
Prior to titration, a 1-2 week washout of any sleeping agent will occur. Titration will then
start with 2.25g at bedtime and then again 4 hours later. This drug may be flexibly
increased to 4.5g (x2 doses) based upon tolerability and effectiveness. We will escalate
dose if drug is toleratedbut without efficacy. Dosing will be increased if subjective sleep
quantity/quality is still reported to be unchanged or if our rating scales indicate minimal
to no change.
After screening visit 1 (eligibility, medical safety determination, washout, sleep EEG)
subjects will return for baseline Visit 2 and start Xyrem.
They will be seen for Visit 3 after 7 days of treatment for rating scales and possible dose
escalation to 6g/d.
They will be seen for Visit 4 after 14 days of treatment for rating scales and possible dose
escalation to 7.5g/d.
They will be seen for Visit 5 after 21 days of treatment for rating scales and possible dose
escalation to 9g/d.
They will be seen for Visit 6/termination after 28 days of treatment for rating scales,
physical exam, lab work, sleep EEG.
Subjects will be called for final safety follow up one week later and 12 weeks later.
Again, liaison with the subject's provider will occur to discuss continuance of Xyrem. If
provider agrees, then long term monitoring will be in the jurisdiction of this provider. If
agreement is to NOT continue Xyrem, patient will be tapered or offered help in finding a
clinician comfortable with the drug. There is no major issue in stopping this drug from a
withdrawal point of view as it does not build up in the system over time in regards to
dependence when used at bed time only. Insomnia will likely return and patient would go back
to their usual treatment if desired and most likely their original level of insomnia.
Safety Measures The overall safety and tolerability of Xyrem will be assessed throughout the
study by adverse event recording, clinical laboratory test results and physical exams. A
Safety monitoring board will consist of the PI and two psychiatry attendings from University
Hospital
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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