Even though there was no significant difference in BMI (P > 0·05) between the CRPS and control groups in this study, the percentage of CRPS patients in our pain clinic who are Trichostatin A price either overweight or obese is higher than the general population [42]. Sleep has been shown to decrease the number of CD14+CD16+ monocytes [40], and
although acute exercise causes a transient increase in CD14+CD16+ monocytes [43,44], individuals who are physically inactive demonstrate a significantly higher percentage of CD14+CD16+ monocytes compared to those who are physically active [41]. Sleeping difficulties and physical inactivity are reported commonly by individuals afflicted with CRPS [4,45]. In addition, we showed that CRPS patients taking antidepressants demonstrated a positive
correlation with elevation of CD14+CD16+ monocytes. Even though other studies have shown that the expression of CD14 and CD16 in monocytes is unchanged in patients with depression compared to normal individuals [46], we cannot rule out that depression or antidepressant use are contributory factors to the increase in CD14+CD16+ monocytes shown by patients with CRPS. Thus, obesity, sleeping difficulties, physical inactivity and possibly depression may be contributory factors leading to the increase in the percentage of CD14+CD16+ monocytes seen in patients with CRPS. Following injury, many individuals develop the signs and PLX4032 ic50 symptoms of CRPS (swelling, buy Hydroxychloroquine redness, allodynia, hyperalgesia, etc.); however, in most patients, normal healing occurs and these signs and symptoms resolve. The process by which a subject fails to undergo normal healing following an injury and progresses to a chronic pain condition as well as the process by which the pain is maintained with little or no chance of resolving are some of the most important
and perplexing questions in CRPS research. The following observations make our finding of elevated CD14+CD16+ proinflammatory monocytes in patients with CRPS relevant to both the initiation and the maintenance of the disease: (1) the activation of microglia and astrocytes has been shown to be both necessary and sufficient for enhanced nociception [13] and (2) blood-borne monocytes/macrophages infiltrate the CNS and differentiate into fully functional microglia [24]. Our data cannot determine whether CD14+CD16+ monocytes were elevated in the study subjects prior to developing CRPS or became elevated afterwards. In either case, independent of causative mechanism, the elevation of blood proinflammatory monocytes prior to the initiating event may predispose individuals for developing the syndrome, whereas the elevation of blood proinflammatory monocytes following the development of CRPS may be relevant for its maintenance. The strengths of this study are: (1) that all patients met strictly defined IASP criteria for CRPS and (2) all patients were diagnosed and examined by the same senior clinician.