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Serum Soluble Interleukin-2 Receptor Does Not Differentiate Complex Regional Pain Syndrome from Other Pain Conditions in a Tertiary Referral Setting

机译:血清可溶性白细胞介素-2受体不会将复杂的区域疼痛综合征与第三节推荐设置中的其他疼痛条件区容化

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Previously, we showed that serum soluble interleukin-2 receptor (sIL-2R) levels, a marker for T-cell activation, were higher in complex regional pain syndrome (CRPS) patients than in healthy controls, suggesting pathogenic T-cell activation in CRPS. Additionally, sIL-2R levels discriminated well between CRPS and healthy controls with a high sensitivity (90%) and specificity (89.5%), suggesting a possible role for sIL-2R in the diagnosis of CRPS. In order to further validate this marker in the diagnostic workup of CRPS, we conducted this prospective cohort study in which we determined sIL-2R levels in patients that were referred to our tertiary referral center with a suspicion of CRPS in a limb, and subsequently compared sIL-2R levels between the patients that were diagnosed with CRPS (CRPS group) and those who were not (no CRPS group). A group of anonymous blood bank donors were used as a healthy control group. Furthermore, we explored the relationship between sIL-2R and CRPS disease severity using the CRPS severity score. Median sIL-2R levels of both the CRPS group (2809.0?pg/ml; Q3-Q1: 3913.0-1589.0) and no CRPS group (3654.0?pg/ml; Q3-Q1: 4429.0-2095.5) were significantly higher than that of the control group (1515.0?pg/ml; Q3-Q1: 1880.0-1150.0): CRPS vs. controls, p.001; no CRPS vs. controls, p0.001. Serum sIL-2R levels did not differ significantly between the CRPS and no CRPS group. A statistically significant negative correlation was observed between sIL-2R levels and the CRPS severity score (rs=?0.468, p=0.024). Our results confirm our previous findings of higher sIL-2R levels in CRPS patients than in healthy controls. We further showed that serum sIL-2R cannot differentiate between CRPS and other pain conditions of a limb in a tertiary referral setting. Interestingly, a negative correlation was found between sIL-2R and CRPS disease severity; this finding warrants further research into the relationship between sIL-2R and CRPS disease severity.
机译:以前,我们表明,复杂的区域疼痛综合征(CRPS)患者的血清可溶性白细胞介素-2受体(SIL-2R)水平,用于T细胞活化的标志物,患者患者高于健康对照,表明CRP中的致病性T细胞活化。此外,SIL-2R水平在CRP和健康对照之间差异,具有高灵敏度(90%)和特异性(89.5%),表明SIL-2R在CRP的诊断中可能作用。为了进一步验证该标记在CRP的诊断次数中,我们进行了这项前瞻性队列研究,其中我们确定了由肢体中的CRP引用的患者的SIL-2R水平,并随后比较了CRP诊断患有CRPS(CRPS组)的患者与未(没有CRPS组)之间的SIL-2R水平。一组匿名血库供体用作健康对照组。此外,我们探讨了使用CRP严重程度得分的SIL-2R与CRPS疾病严重程度之间的关系。 CRP组的中位SIL-2R水平(2809.0?PG / mL; Q3-Q1:3913.0-1589.0)和无CRPS组(3654.0〜PG / ml; Q3-Q1:4429.0-2095.5)显着高于对照组(1515.0?pg / ml; Q3-Q1:1880.0-1150.0):CRP与控制,P <.001;没有CRPS对照,P <0.001。 CRP和NO CRPS组之间的血清SIL-2R水平没有显着差异。在SIL-2R水平和CRPS严重程度之间观察到统计学上显着的负相关(RS = 0.468,P = 0.024)。我们的结果证实了我们之前的CRP患者中的高级SIL-2R水平的发现,而不是健康的控制。我们进一步表明,血清SIL-2R不能在第三推荐设置中区分CRP和其他止血条件。有趣的是,SIL-2R和CRPS疾病严重程度之间发现了负相关性;这一发现认证进一步研究SIL-2R和CRPS疾病严重程度之间的关系。

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