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A randomized double-blind placebo-controlled trial of the effectiveness of melatonin on neurocognition and sleep in survivors of childhood cancer.

Pediatric blood & cancer
January 1, 2022
Margaret M Lubas et al. (13 authors)
Journal ArticleRandomized Controlled TrialResearch Support, N.I.H., ExtramuralResearch Support, Non-U.S. Gov'tHuman StudyClinical
Study Details

Study Goal

The researchers aimed to determine whether melatonin improves neurocognitive performance and sleep in adult survivors of childhood cancer with neurocognitive and/or sleep impairments.

Results Summary

Intent-to-treat analyses showed no significant overall improvements in neurocognitive performance or sleep, but subsets of survivors with specific impairments (neurocognitive or sleep-only) demonstrated clinically significant treatment responses in certain domains like visuomotor speed, nonverbal reasoning, shifting attention, short-term memory, and sleep duration.

Population

Adult survivors of childhood cancer (mean age 33.5 years, 26 years post-diagnosis) with neurocognitive and/or sleep impairments.

Effective Dosage

3 mg time-release melatonin.

Duration

Six months.

Interactions

None mentioned.

Extracted Claims (7)
InterventionDirectionEndpointPopulationDosageImpactClaim #
3 mg time-release melatonin
no change
neurocognitive performance
survivors from the St. Jude Lifetime Cohort
no statistically significant differences
no statistically significant differences
#1
3 mg time-release melatonin
no change
sleep
survivors from the St. Jude Lifetime Cohort
no statistically significant differences
no statistically significant differences
#2
3 mg time-release melatonin
increase
visuomotor speed
survivors with neurocognitive impairment only
63% vs 41%
a larger proportion demonstrated a treatment response
#3
3 mg time-release melatonin
increase
nonverbal reasoning
survivors with neurocognitive impairment only
46% vs 28%
a larger proportion demonstrated a treatment response
#4
3 mg time-release melatonin
increase
shifting attention
survivors with sleep impairment only
44% vs 28%
a larger proportion demonstrated a treatment response
#5
3 mg time-release melatonin
increase
short-term memory
survivors with sleep impairment only
39% vs 19%
a larger proportion demonstrated a treatment response
#6
3 mg time-release melatonin
increase
actigraphy-assessed sleep duration
survivors with sleep impairment only
47% vs 29%
a larger proportion demonstrated a treatment response
#7
Abstract

BACKGROUND: Adult survivors of childhood cancer are at risk of developing sleep and neurocognitive problems, yet few efficacious interventions exist targeting these prevalent late effects. Melatonin has known sleep-promoting effects; however, it has not been well studied among childhood cancer survivors. METHOD: Survivors (n = 580; mean age = 33.5 years; 26 years post-diagnosis) from the St. Jude Lifetime Cohort were randomized (1:1) to a six-month double-blind placebo-controlled trial of 3 mg time-release melatonin within three strata (stratum 1: neurocognitive impairment only; stratum 2: neurocognitive and sleep impairment; stratum 3: sleep impairment only). Neurocognitive performance was assessed at baseline and post-intervention using standardized measures. Sleep was assessed via self-report and actigraphy. Independent sample t tests compared mean change scores from baseline to six months. Post-hoc analyses compared the prevalence of clinically significant treatment responders among melatonin and placebo conditions within and across strata. RESULTS: Intent-to-treat analyses revealed no statistically significant differences in neurocognitive performance or sleep from baseline to post-intervention. However, among survivors with neurocognitive impairment only, a larger proportion randomized to melatonin versus placebo demonstrated a treatment response for visuomotor speed (63% vs 41%, P = 0.02) and nonverbal reasoning (46% vs 28%, P = 0.04). Among survivors with sleep impairment only, a larger proportion treated with melatonin demonstrated a treatment response for shifting attention (44% vs 28%, P = 0.05), short-term memory (39% vs 19%, P = 0.01), and actigraphy-assessed sleep duration (47% vs 29%, P = 0.05). CONCLUSION: Melatonin was not associated with improved neurocognitive performance or sleep in our intent-to-treat analyses; however, a subset of survivors demonstrated a clinically significant treatment response.

Medical Subject Headings (MeSH)
AdultCancer SurvivorsChildDouble-Blind MethodHumansMelatoninNeoplasmsSleepSurvivors
Study Links
Quality Scores
SafetyNot Assessed
Efficacy65/10
Quality85/10
Citation Metrics
Total Citations3
Citations/Year1.0
Relative Citation Ratio0.27
NIH Percentile14.1%
Research Impact Scores
APT Score0.25
Weight Score2.52
Normalized Score0.63
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