Posttraumatic Stress Disorder Clinical Trial
Official title:
A Psychophysiologic Study of Weakening Traumatic Combat Memories With Post-Reactivation Propranolol
The consolidation of learning is enhanced by adrenalin and other stress hormones. This
memory enhancing effect is opposed by propranolol. In posttraumatic stress disorder (PTSD),
a psychologically traumatic event may overstimulate stress hormones such as adrenalin, which
in turn overly strengthen consolidation of the memory of the event, leading to an
excessively powerful and persistent memory. Administration of propranolol after a
psychologically traumatic event could reduce subsequent PTSD. Unfortunately, there exists a
window of opportunity for influencing the consolidation of a traumatic event into long-term
memory. In persons who have already developed PTSD, this would have closed months or years
earlier. However, recent developments in animal research suggest that reactivation
(retrieval) of a consolidated memory can return it to a labile state, from which it must be
restabilized in order to persist. This process, which has been termed "reconsolidation," can
be reduced in animals by propranolol.
In a preliminary study performed by the PI and colleagues in Canada, civilian participants
with PTSD described the traumatic event during a script preparation session, which served to
reactivate their traumatic memory. They then received either propranolol or placebo. A week
later, during script-driven imagery of their traumatic events, physiologic responses were
smaller in the participants who had received post-reactivation propranolol compared to
placebo, suggesting that the traumatic memory had been weakened by the propranolol. These
results suggest that that post-reactivation propranolol recapitulates its effects on
consolidation, this time by blocking reconsolidation of the traumatic memory.
Several important questions remain unanswered. First, does propranolol also weaken traumatic
memories in combat-related PTSD? Second, does this weakening effect only occur when the
propranolol is given after combat memory reactivation? If not, this would refute the
reconsolidation hypothesis and suggest that propranolol affects non-specific mechanisms.
Third, how long does the traumatic memory weakening last?
The proposed project will investigate these questions by performing an improved,
double-blind, placebo-controlled study in Iraq and Afghanistan veterans with combat-related
PTSD. Participants will be randomly assigned to one of two groups: post-reactivation
propranolol or non-reactivation propranolol. Participants in the non-reactivation
propranolol group will receive propranolol in the absence of traumatic memory reactivation.
Participants randomized to the post-reactivation propranolol group will receive matching
placebo capsules. Two days later, all participants will return for a script preparation
session, at which time they will describe the details of their traumatic event. Participants
randomized to the post-reactivation propranolol group will then receive propranolol, whereas
participants randomized to the non-reactivation propranolol group will receive placebo.
Participants will then return for psychophysiologic script-driven imagery testing one week
and six months later. We hypothesize that those who receive propranolol after reactivation
of their memories of their traumatic combat event(s) will show significantly smaller
psychophysiologic responses during script-driven imagery testing compared to participants
who receive propranolol in the absence of combat memory reactivation, supporting the
inference that post-reactivation propranolol blocks the reconsolidation of traumatic combat
memories.
Background: Animal evidence indicates that some consolidated memories when reactivated
(retrieved) need to be reconsolidated. During this process, memories can be enhanced or
weakened. In a preliminary, randomized, double-blind, placebo-controlled study, we tested
whether post-reactivation administration of the beta-adrenergic blocker propranolol, which
reduces reconsolidation of aversive memories in rodents, would reduce the emotional strength
of traumatic memories, or conditioned fear responses, in patients with non-combat-related
PTSD. Civilian participants described their traumatic event during a "script preparation"
session and thereafter received either a combined dose of short- and long-acting propranolol
(n=9), or placebo (n=10). A week later, they engaged in script-driven mental imagery of
their personal traumatic events, while peripheral physiologic responses were recorded as
measures of the emotional strength of the traumatic memory. We found that physiologic
responses were significantly smaller in the participants who had received post-reactivation
propranolol compared to placebo a week earlier: F(3,15)=5.1, p=.007, η2=.49. The results of
this preliminary study are consistent with pharmacologic blockade of reconsolidation of
traumatic memories in PTSD. However, several important questions remain unanswered. First,
does propranolol also weaken traumatic memories in combat-related PTSD? Second, does this
weakening effect only occur when the propranolol is given when combined with traumatic
memory reactivation? If not, this would refute the reconsolidation hypothesis and suggest
that propranolol affects non-specific mechanisms. Third, how long does the traumatic memory
weakening last, i.e., does recovery of the conditioned fear response occur?
Objective/Hypothesis: The first objective is to replicate and extend the finding from the
preliminary study to Iraq and Afghanistan combat veterans with PTSD by showing that
propranolol following combat memory reactivation results in a significantly greater
weakening of traumatic combat memories than propranolol alone, supporting the proposition
that this weakening is due to pharmacological blockade of memory reconsolidation, rather
than non-specific actions of propranolol. We hypothesize that participants who undergo
script preparation for the combat event(s) that caused their PTSD, followed by
(post-reactivation) propranolol, will show significantly smaller psychophysiologic responses
during script-driven imagery testing a week later compared to those who receive
(non-reactivation) propranolol two days prior to combat script preparation. The second
objective to show that this effect is long-lasting, which would be expected if the
underlying mechanism is reduction of the traumatic memory trace by blockade of
reconsolidation. We hypothesize that the effect will remain significant when participants
undergo follow-up psychophysiologic script-driven imagery testing six months later.
Specific Aim: To perform a controlled, randomized, double-blind study in Iraq and
Afghanistan veterans with combat-related PTSD that addresses the above hypotheses.
Study Design: Participants will be randomly assigned to one of two groups: post-reactivation
propranolol or non-reactivation propranolol. After written informed consent is obtained,
participants randomized to the non-reactivation propranolol group will receive a "test" dose
of 0.67 mg/kg short-acting propranolol combined with 1 mg/kg long-acting propranolol.
Participants randomized to the post-reactivation propranolol group will receive matching
placebo capsules. Two days later, all participants will return for an approximate 15-30
minute "script preparation" session, at which time they will describe the details of their
traumatic combat event(s) to the Principal Investigator. Participants randomized to the
post-reactivation propranolol group will then receive the combined propranolol dose, whereas
participants randomized to the non-reactivation propranolol group will receive placebo.
Based upon the history obtained during the script preparation session, the Principal
Investigator will compose "scripts" approximately 30 seconds in duration portraying each
participant's combat events in their own words. Participants will then return for
script-driven imagery testing sessions in the psychophysiology laboratory one week and six
months later. During each of these sessions, they will undergo recording of heart rate, skin
conductance, and corrugator and frontalis electromyogram during a baseline period. They will
then listen to a recording of their traumatic scripts and be instructed to imagine the
events portrayed as if they were happening again, while physiologic measures are recorded.
Responses (change) scores for each physiologic variable for each session will be calculated
by subtracting the preceding baseline period mean from the imagery period mean. The
physiologic data will be analyzed by multivariate analysis of variance (MANOVA) followed by
univariate ANOVAs. The hypothesis predicts that at each time period, the physiologic
responses of the post-reactivation propranolol group will be significantly smaller than
those of the non-reactivation propranolol group.
Relevance: If a traumatic memory undergoes reconsolidation when reactivated, this could
re-open the window of opportunity to influence the memory pharmacologically. This could have
important implications for the treatment of PTSD. Should the proposed psychophysiologic
study confirm that post-reactivation propranolol weakens traumatic combat memories, it would
be a relatively short leap to clinical studies of the therapeutic efficacy of this novel
modality.
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