A four-week dose titration of prazosin or placebo was followed by

A four-week dose titration of prazosin or placebo was followed by 8 weeks of maintenance medication (maximum

bedtime dose = 15 mg; mean maintenance bedtime prazosin dose = 13.3 mg). Prazosin was significantly and substantially superior to placebo for reducing nightmares and sleep disturbance and improving global clinical status. Dream content was assessed using the PTSD Dream Rating Scale (Tian et al., 2014), demonstrating a change from those typical of trauma nightmares toward those typical of normal dreaming. The third RCT was performed by Germain and colleagues (Germain et al., 2012) in which 50 PTSD veterans with chronic sleep disturbance were randomized to one of three conditions: prazosin (mean dose = 9 mg at night); a behavioral sleep intervention (BSI) that included imagery rehearsal therapy,

stimulus control and sleep restriction; Sunitinib molecular weight or placebo pill treatment. Both prazosin and BSI were significantly more EGFR activation effective than placebo for sleep improvement, reduction in both nocturnal and daytime PTSD symptoms and improvement of global function. The fourth RCT was performed in active duty American soldiers returned from combat deployments in Iraq and Afghanistan (Raskind et al., 2013). Because prazosin duration of action is approximately 6–10 h, a midmorning prazosin dose was included as well as a larger bedtime prazosin dose to address daytime PTSD symptoms. Maintenance prazosin doses were 4.0 ± 1.2 mg midmorning and 15.6 ± 6.0 mg bedtime for men; and 2.0 ± 0.0 mg midmorning and 7.0 ± 3.5 mg bedtime for women. Prazosin was significantly more effective than placebo for reducing CAPS “recurrent distressing dreams of the event” item scores; Pittsburgh Sleep Quality Index scores; and total 17 item CAPS scores (reduction from baseline = 25.1 ± 3.4 prazosin group and 13.8 ± 3.3 placebo group [(p = 0.02]). Total CAPS score decrease remained significantly greater in the prazosin group (p = 0.04) even after removing the nightmare item. Similar open label

prazosin beneficial effects with good tolerability have been reported in soldiers performing combat operations in the dehydrating Iraq desert warfare environment ( Calohan et al., 2010), and in elderly World War II Veterans and Holocaust survivors ( Peskind et al., 2003). Studies heptaminol of civilians with PTSD have examined nighttime as well as daytime administration of prazosin. A double-blind placebo crossover design study found that nighttime prazosin significantly reduced subjective PTSD symptoms of trauma-relevant nightmares and insomnia while preserving normal dreaming (Taylor et al., 2008). Subjective measures of sleep were also recorded using a portable monitoring device allowing participants to sleep in their own homes thus avoiding confounding variables associated with sleep lab monitoring. Compared with placebo, prazosin significantly increased total sleep time, REM sleep time, and mean REM period duration in the absence of a sedative-like effect on sleep onset latency (Taylor et al., 2008).

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