PTSD Clinical Trial
Official title:
Evaluation of the Efficacy of the NK1 Antagonist GR205171 in Posttraumatic Stress Disorder
This study, conducted at the NIH and the Mount Sinai School of Medicine, will examine the
effectiveness of a substance P or NK1 antagonist study drug known as GR205171 in treating the
symptoms of posttraumatic stress disorder (PTSD).
People between 18 and 65 years of age who have been diagnosed with PTSD may be eligible for
this study. Participants undergo the following tests and procedures:
Treatment: Patients are tapered off current ineffective medications over 1 to 2 weeks. All
participants receive placebo (sugar pill) at the start of the study. At some point within the
first 3 weeks of the study, they are then randomly assigned either to take GR205171 or to
continue with placebo for the remainder of the 10-week treatment period.
Clinic visits: Patients come to the clinic once a week during treatment. The following
procedures are done at various visits.
- Interviews, self report questionnaires and psychiatric rating scales at every visit.
- Physical examination, blood and urine tests. Blood is drawn up to 10 times during the
study.
Follow-up visits continue for up to 3 months after the end of the study, during which
patients are offered standard clinical treatment.
Posttraumatic Stress Disorder (PTSD) is a common chronic anxiety disorder that is often
debilitating and follows exposure to an overwhelming traumatic event. The burden of PTSD on
individuals and society is significant. The majority of PTSD sufferers also meet the
diagnostic criteria for several other psychiatric disorders and many attempt suicide. Despite
the devastating impact of PTSD on the lives of millions worldwide, little is known about the
etiology or pathophysiology of this disorder. Although disruptions in the
hypothalamic-pituitary adrenal (HPA) Axis, noradrenergic, serotonergic systems have been
proposed as neurobiological substrates in the development of PTSD, the exact underpinnings of
the neurobiology of PTSD remain to be fully elucidated.
PTSD is responsive to treatment with selective serotonin reuptake inhibitors, but response
rates rarely exceed 60%, and even fewer patients (20%-30%) experience improvement that could
be characterized as remission. Thus, there is a clear need to develop novel and improved
therapeutics for PTSD. A growing body of preclinical evidence suggests that activation of the
Substance P (SP) and its receptor NK1 is anxiogenic and that NK1 antagonists, upon chronic
administration, exert significant dampening (albeit complex) effects on the SP-NP system.
Furthermore, several stress paradigms are believed to exert many of their deleterious effects
on hippocampal structures via enhancement of SP-NK1 system. Overall, excess activity of the
SP-NK1 system stands as a prime candidate for involvement in the pathophysiology of anxiety
disorders such as PTSD.
In this study, we propose to investigate the potential antianxiety efficacy of the highly
specific NK1 antagonist GR205171 in PTSD. Furthermore, we propose to, in a preliminary
fashion, longitudinally investigate whether neuroendocrine surrogate markers are predictive
of treatment response.
This is an 8-week double-blind placebo-controlled study that will examine the efficacy and
safety of an NK1 antagonist in patients with PTSD.
Patients, ages 18 to 65 years with a diagnosis of PTSD, will in this pilot study be
randomized to double-blind treatment to receive either the NK1 antagonist, GR205171 (5
mg/day) or placebo for a period of 8 weeks.
Approximately 52 patients will enter the study to obtain 40 subjects who complete the 8 weeks
of acute NK1 antagonist treatment.
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