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健康受试者唾液中潜在疼痛生物标志物的可靠性:个体间差异和不同检测时段的变异性

Reliability of Potential Pain Biomarkers in the Saliva of Healthy Subjects: Inter-Individual Differences and Intersession Variability.

作者信息

Sobas Eva M, Reinoso Roberto, Cuadrado-Asensio Rubén, Fernández Itziar, Maldonado Miguel J, Pastor José C

机构信息

Instituto Universitario de Oftalmobiología Aplicada (IOBA), Universidad de Valladolid, Valladolid, Spain.

Escuela de Enfermería, Universidad de Valladolid, Valladolid, Spain.

出版信息

PLoS One. 2016 Dec 1;11(12):e0166976. doi: 10.1371/journal.pone.0166976. eCollection 2016.

Abstract

AIM

Salivary cortisol, α-amylase (sAA), secretory IgA (sIgA), testosterone, and soluble fraction of receptor II of TNFα (sTNFαRII) could serve as objective pain measures, but the normal variability of these potential biomarkers is unknown.

PATIENTS & METHODS: Saliva was collected with the passive secretion method from 34, pain-free subjects in two single samples at least 24 hours apart. Biomarker variation and intersession reliability were assessed with the intraclass correlation coefficient (ICC). Also, we calculated the within-subject standard deviation (Sw) and the reproducibility (2.77 × Sw) of intersession measures.

RESULTS

Salivary cortisol, sAA, sIgA, testosterone, and sTNFαRII yielded the following ICCs: 0.53, 0.003, 0.88, 0.42 and 0.83, respectively. We found no statistically significant systematic differences between sessions in any biomarker except for testosterone, which showed a decrease on the second day (p<0.001). The reproducibility for salivary cortisol, sAA, sIgA, testosterone, and sTNFαRII were 0.46 ng/ml, 12.88 U/ml, 11.7 μg/ml, 14.54 pg/ml and 18.29 pg/ml, respectively. Cortisol, testosterone and TNFαRII measurement variability showed a positive correlation with the magnitude (p<0.002), but no relationship was found for sAA and sIgA.

CONCLUSIONS

Salivary sIgA and sTNFαRII show a remarkable good reproducibility and, therefore, could be useful as pain biomarkers. When using the passive secretion method, intersession variations in salivary sIgA of more than 11.7 μg/ml may reflect true biomarker change. In the case of sTNFαRII this will depend of the magnitude. The estimates herein provided should help investigators and clinicians differentiate actual biomarker modification from measurement variability.

摘要

目的

唾液皮质醇、α-淀粉酶(sAA)、分泌型免疫球蛋白A(sIgA)、睾酮以及肿瘤坏死因子α受体II的可溶性部分(sTNFαRII)可作为客观的疼痛指标,但这些潜在生物标志物的正常变异性尚不清楚。

患者与方法

采用被动分泌法,从34名无疼痛的受试者中采集唾液,分两个单次样本采集,间隔至少24小时。使用组内相关系数(ICC)评估生物标志物的变异性和不同时间段之间的可靠性。此外,我们还计算了受试者内标准差(Sw)和不同时间段测量的可重复性(2.77×Sw)。

结果

唾液皮质醇、sAA、sIgA、睾酮和sTNFαRII的ICC分别为:0.53、0.003、0.88、0.42和0.83。除睾酮在第二天有所下降(p<0.001)外,我们发现任何生物标志物在不同时间段之间均无统计学上的显著系统性差异。唾液皮质醇、sAA、sIgA、睾酮和sTNFαRII的可重复性分别为0.46 ng/ml、12.88 U/ml、11.7 μg/ml、14.54 pg/ml和18.29 pg/ml。皮质醇、睾酮和TNFαRII测量变异性与测量值大小呈正相关(p<0.002),但未发现sAA和sIgA存在相关性。

结论

唾液sIgA和sTNFαRII具有显著良好的可重复性,因此可作为疼痛生物标志物。采用被动分泌法时,唾液sIgA不同时间段变化超过11.7 μg/ml可能反映生物标志物的真实变化。对于sTNFαRII,这将取决于测量值大小。本文提供的估计值应有助于研究人员和临床医生区分生物标志物的实际变化与测量变异性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7188/5132231/bf36d79152dc/pone.0166976.g001.jpg

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