Qian Li, Yuanshao Lin, Wensi Huang, Yulei Zhou, Xiaoli Chen, Brian Wang, Wanli Zhang, Zhengyi Cai, Jie Xue, Wenhui Zhang, Tieer Yu, Hong Wang, Jincai He, Kunlin Jin, Bei Shao
1Zhejiang Provincial Key Laboratory of Aging and Neurological Disorder Research.
3Institute for Healthy Aging, Center for Neuroscience Discovery, University of North Texas Health Science Center, Fort Worth, Texas 76107, USA.
Aging Dis. 2016 Oct 1;7(5):614-622. doi: 10.14336/AD.2016.0207. eCollection 2016 Oct.
Interleukin-33 (IL-33), a newly recognized IL-1 family member, is expressed in various tissues and cells, and involved in pathogenesis of many human diseases. For example, IL-33 plays a protective role in cardiovascular diseases. However, the role of IL-33 in acute ischemic stroke (AIS) remains unclear. This study aims to investigate whether IL-33 level in AIS patient serum can be used as a potential diagnostic and prognostic marker. The study included two hundred and six patients with first-ever ischemic stroke, who were admitted within 72 hours after stroke onset. The serum level of IL-33 was measured with ELISA and the severity of AIS patients on admission was evaluated based on the National Institutes of Health Stroke Scale (NIHSS) score. The functional outcome at 3 months was determined using the Barthel index (BI). We found that serum IL-33 was significantly higher ( < 0.001) in patients with AIS [57.68 ng/L (IQR, 44.95-76.73)] compared with healthy controls [47.48 ng/L (IQR, 38.67-53.78)]. IL-33 was an independent diagnostic biomarker for AIS with an OR of 1.051 (95%Cl, 1.018-1.085; P=0.002). Serum IL-33 was higher ( < 0.05) in the stroke patients with small cerebral infarction volume compared to AIS patients with large cerebral infarction. In addition, serum IL-33 was also significantly higher ( = 0.001) in the patients with mild stroke, compared to the patients with severe stroke. Furthermore, serum IL-33 level in AIS patients with a worse outcome was higher ( < 0.001) compared to AIS patients with a better outcome. IL-33 was also an independent predictor for the functional outcome with an adjusted OR of 0.932 (95% CI, 0.882-0.986). Our results suggest that the lower level of serum IL-33 is associated with large infarction volume and greater stroke severity in AIS patients. Thus, IL-33 can be used as a novel and independent diagnostic and predicting prognostic marker in AIS.
白细胞介素-33(IL-33)是一种新发现的白细胞介素-1家族成员,在多种组织和细胞中表达,并参与多种人类疾病的发病机制。例如,IL-33在心血管疾病中发挥保护作用。然而,IL-33在急性缺血性卒中(AIS)中的作用仍不清楚。本研究旨在探讨AIS患者血清中的IL-33水平是否可作为潜在的诊断和预后标志物。该研究纳入了206例首次发生缺血性卒中的患者,这些患者在卒中发作后72小时内入院。采用酶联免疫吸附测定法(ELISA)检测IL-33的血清水平,并根据美国国立卫生研究院卒中量表(NIHSS)评分评估AIS患者入院时的严重程度。使用巴氏指数(BI)确定3个月时的功能结局。我们发现,与健康对照者[47.48 ng/L(四分位间距,38.67 - 53.78)]相比,AIS患者[57.68 ng/L(四分位间距,44.95 - 76.73)]的血清IL-33显著更高(<0.001)。IL-33是AIS的独立诊断生物标志物,比值比为1.051(95%置信区间,1.018 - 1.085;P = 0.002)。与大脑梗死体积大的AIS患者相比,大脑梗死体积小的卒中患者血清IL-33更高(<0.05)。此外,与重度卒中患者相比,轻度卒中患者的血清IL-33也显著更高(=0.001)。此外,与结局较好的AIS患者相比,结局较差的AIS患者血清IL-33水平更高(<0.001)。IL-33也是功能结局的独立预测因子,校正后的比值比为0.932(95%置信区间,0.882 - 0.986)。我们的结果表明,血清IL-33水平较低与AIS患者梗死体积大及卒中严重程度更高有关。因此,IL-33可作为AIS一种新的独立诊断和预测预后的标志物。
