The journal of pain : official journal of the American Pain Society
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Multicenter Study Comparative Study
Does the Neonatal Facial Coding System differentiate between infants experiencing pain-related and non-pain-related distress?
The Neonatal Facial Coding System (NFCS) is widely accepted as a measure of infant pain-related distress in known pain-specific contexts. It has clearly shown the ability to distinguish between facial reactivity in no-pain and pain-related situations. The primary purpose of this study was to explore whether NFCS differentiates between pain-related and non-pain-related distress. Two groups of 35 infants (1 group was distressed before injection whereas the other group was not distressed before injection) were coded using NFCS before and after an immunization procedure. Within-group analyses of infants who were distressed before immunization suggested that NFCS was not able to discriminate between pain-related and non-pain-related distress. However, between-group analyses showed NFCS discriminated between potential gradations of distress in infants after immunization. Results suggest that NFCS has the ability to discriminate between intensities of distress but not between pain-related and non-pain-related distress. ⋯ Adding to the NFCS validity literature, this study suggests that while able to distinguish between no-distress and pain-related distress, facial actions of NFCS may not distinguish between pain-related and non-pain-related distress expressions. However, NFCS was able to discern infants presumed to have higher pain-related distress due to experiencing pre-needle distress.
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Multicenter Study Clinical Trial
A single-blind, placebo run-in study of duloxetine for activity-limiting osteoarthritis pain.
Osteoarthritis pain is a significant problem for our aging population. Antidepressants that are serotonin-norepinephrine reuptake inhibitors are effective for other forms of chronic pain and may provide a new treatment option for osteoarthritis pain. We performed a single-blind, placebo run-in trial of 60 to 90 mg of duloxetine in 25 subjects with activity-limiting osteoarthritis pain. Each subject received 2 weeks of placebo followed by 10 weeks of duloxetine. The primary outcome was reduction in average pain intensity between 2 and 12 weeks for subjects completing the trial. Average pain on the Brief Pain Inventory (BPI) was 5.7 at baseline, 4.8 after the 2-week placebo run-in, and 3.5 at 12 weeks for the 17 patients completing the trial (28% decrease between 2 and 12 weeks, P = .122). Eight of 15 study completers who had nonmissing BPI results (53%) reported at least 30% pain reduction between weeks 2 and 12. The Western Ontario McMaster Osteoarthritis Index (WOMAC) pain score at baseline was 2.3, 1.8 after 2 weeks, and 1.3 after 12 weeks (30% decrease between 2 and 12 weeks, P = .018). Ten of 17 patients (59%) reported at least 30% pain relief between weeks 2 and 12 on the WOMAC. Significant improvements in self-reported physical and role function were reported but observed physical function did not improve. ⋯ Duloxetine did not significantly reduce pain intensity on the BPI but did improve pain intensity and self-reported function on the WOMAC. Duloxetine warrants further investigation as a novel treatment for osteoarthritis pain.