Patel Neil, Belcher John, Thorpe Gary, Forsyth Nicholas R, Spiteri Monica A
Department of Respiratory Medicine, University Hospitals of North Midlands NHS Trust, Ground Floor, Trent Building, Newcastle Road, Stoke-on-Trent, ST4 6QG, UK.
School of Computing and Mathematics, Keele University, Stoke-on-Trent, Staffordshire.
Respir Res. 2015 May 28;16(1):62. doi: 10.1186/s12931-015-0219-1.
Saliva is increasingly promoted as an alternative diagnostic bio-sample to blood; however its role in respiratory disease requires elucidation. Our aim was to investigate whether C-reactive protein (CRP), procalcitonin (PCT) and neutrophil elastase (NE) could be measured in unstimulated whole saliva, and to explore differences between COPD patients and controls with normal lung function. We also determined the relationship between these salivary biomarkers and self-reported COPD-relevant metrics.
Salivary CRP, PCT and NE levels were measured at each of 3 visits over a 14-day period alongside spirometry and a daily self-assessment dairy in 143 subjects: 20 never-smokers and 25 smokers with normal spirometry; 98 COPD patients [GOLD Stage I, 16; Stage II, 32; Stage III, 39; Stage IV, 11]. Twenty-two randomly selected subjects provided simultaneous blood samples.
Levels of each salivary biomarker could distinguish between the above cohorts. Significant differences remained for salivary CRP and NE (p < 0.05) following adjustment for age, gender, sampling time, gum disease and total co-morbidities; but not for BMI except for salivary NE, which remained higher in smokers compared to non-smokers and stable COPD subjects (p < 0.001). Patients with acute COPD exacerbations had a median increase in all 3 salivary biomarkers (p < 0.001); CRP: median 5.74 ng/ml, [interquartile range (IQR) 2.86-12.25], PCT 0.38 ng/ml, [IQR 0.22-0.94], and NE 539 ng/ml, [IQR 112.25-1264]. In COPD patients, only salivary CRP and PCT levels correlated with breathing scores (r = 0.14, p < 0.02; r = 0.13, p < 0.03 respectively) and sputum features but not with activities of daily living. Salivary CRP and PCT concentrations strongly correlated with serum counterparts [r = 0.82, (95% CI: 0.72-0.87), p < 0.001 by Spearman's; and r = 0.53, (95% CI: 0.33-0.69), p < 0.006 respectively]; salivary NE did not.
CRP, PCT and NE were reliably and reproducibly measured in saliva, providing clinically-relevant information on health status in COPD; additionally NE distinguished smoking status. All 3 salivary biomarkers increased during COPD exacerbations, with CRP and PCT correlating well with patient-derived clinical metrics. These results provide the conceptual basis for further development of saliva as a viable bio-sample in COPD monitoring and exacerbation management.
唾液作为一种替代血液的诊断生物样本,其应用正日益受到推广;然而,唾液在呼吸系统疾病中的作用尚需阐明。我们的目的是研究是否可以在未刺激的全唾液中检测C反应蛋白(CRP)、降钙素原(PCT)和中性粒细胞弹性蛋白酶(NE),并探讨慢性阻塞性肺疾病(COPD)患者与肺功能正常的对照组之间的差异。我们还确定了这些唾液生物标志物与自我报告的COPD相关指标之间的关系。
在14天内的3次就诊中,对143名受试者进行唾液CRP、PCT和NE水平的检测,同时进行肺功能测定和每日自我评估记录,这些受试者包括:20名从不吸烟者和25名肺功能正常的吸烟者;98名COPD患者[全球慢性阻塞性肺疾病倡议(GOLD)I期,16例;II期,32例;III期,39例;IV期,11例]。随机选取22名受试者同时采集血液样本。
每种唾液生物标志物的水平能够区分上述队列。在对年龄、性别、采样时间、牙龈疾病和总合并症进行校正后,唾液CRP和NE仍存在显著差异(p<0.05);除唾液NE外,体重指数(BMI)无显著差异,吸烟者的唾液NE水平高于非吸烟者和稳定期COPD患者(p<0.001)。COPD急性加重患者的所有3种唾液生物标志物中位数均升高(p<0.001);CRP:中位数5.74 ng/ml,[四分位数间距(IQR)2.86 - 12.25],PCT 0.38 ng/ml,[IQR 0.22 - 0.94],NE 539 ng/ml,[IQR 112.25 - 1264]。在COPD患者中,只有唾液CRP和PCT水平与呼吸评分相关(r = 0.14,p<0.02;r = 0.13,p<0.03)以及与痰液特征相关,但与日常生活活动无关。唾液CRP和PCT浓度与血清对应物高度相关[r = 0.82,(95%置信区间:0.72 - 0.87),Spearman检验p<0.001;r = 0.53,(95%置信区间:0.33 - 0.69),p<0.006];唾液NE则不然。
在唾液中可可靠且可重复地检测到CRP、PCT和NE,为COPD的健康状况提供了临床相关信息;此外,NE可区分吸烟状态。在COPD急性加重期间,所有3种唾液生物标志物均升高,CRP和PCT与患者的临床指标相关性良好。这些结果为进一步开发唾液作为COPD监测和急性加重管理中可行的生物样本提供了概念基础。
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