RT Journal Article
SR Electronic
T1 Ethnic Differences Identified by Pain Sensitivity Questionnaire Correlate With Clinical Pain Responses
JF Regional Anesthesia &amp; Pain Medicine
JO Reg Anesth Pain Med
FD BMJ Publishing Group Ltd
SP 200
OP 204
DO 10.1097/AAP.0000000000000689
VO 43
IS 2
A1 Brooke A. Bell
A1 Ruth Ruscheweyh
A1 Bernard Joseph Kelley
A1 Timothy J. Ness
A1 Thomas R. Vetter
A1 Alethia Baldwin Sellers
YR 2018
UL http://rapm.bmj.com/content/43/2/200.abstract
AB Background and Objectives The Pain Sensitivity Questionnaire, English version (PSQ-E), is predictive of pain-related responses to experimental stimuli. Ethnic differences have been noted in experimental measures of pain sensation using quantitative sensory testing. The present study sought to determine if the PSQ-E also identified similar ethnic differences.Methods Fifty-seven subjects who self-identified as African Americans (AAs) and who were scheduled to undergo a low-back interventional procedure completed the PSQ-E and other questionnaires. Their data were compared with an age-, sex-, and opioid usage–matched sample of 57 self-identified non-Hispanic white (NHW) subjects. Pain ratings on a visual analog scale (VAS) were obtained following 2 standardized injections of subcutaneous lidocaine (VAS1—infiltration in hand, VAS2—infiltration of procedural site). Correlations between PSQ-E scores, VAS measures, and other inventories were tested.Results The PSQ-E scores and clinical and experimental pain scores were all significantly elevated in AA compared with NHW patients (P &lt; 0.05 for experimental pain scores, P &lt; 0.001 for PSQ and clinical pain scores). Measures of pain interference, depression, anxiety, and pain catastrophizing were not different between groups. Similar to our previous study, PSQ-E scores significantly correlated with both experimental and clinical pain scores (eg, PSQ-E with Brief Pain Inventory pain score: r = 0.39, P &lt; 0.001).Conclusions The study demonstrated significantly elevated pain sensitivity in AA compared with NHW patients as measured by the PSQ-E and experimental and clinical pain intensity scores. This shows that the PSQ reflects the known elevation of pain sensitivity in AA subjects and suggests that it may be useful in assessing pain treatment disparities by identifying and standardizing differences in pain sensitivity.