Emsley Hedley C A, Smith Craig J, Gavin Carole M, Georgiou Rachel F, Vail Andy, Barberan Elisa M, Illingworth Karen, Scarth Sylvia, Wickramasinghe Vijitha, Hoadley Margaret E, Rothwell Nancy J, Tyrrell Pippa J, Hopkins Stephen J
Division of Neuroscience, The University of Liverpool, The Walton Centre for Neurology & Neurosurgery, Lower Lane, Liverpool L9 7LJ, UK.
BMC Neurol. 2007 Feb 28;7:5. doi: 10.1186/1471-2377-7-5.
As critical mediators of local and systemic inflammatory responses, cytokines are produced in the brain following ischaemic stroke. Some have been detected in the circulation of stroke patients, but their role and source is unclear. Focusing primarily on interleukin(IL)-1-related mechanisms, we serially measured plasma inflammatory markers, and the production of cytokines by whole blood, from 36 patients recruited within 12 h and followed up to 1 year after acute ischaemic stroke (AIS).
Admission plasma IL-1 receptor antagonist (IL-1ra) concentration was elevated, relative to age-, sex-, and atherosclerosis-matched controls. IL-1beta, soluble IL-1 receptor type II, tumour necrosis factor (TNF)-alpha, TNF-RII, IL-10 and leptin concentrations did not significantly differ from controls, but peak soluble TNF receptor type I (sTNF-RI) in the first week correlated strongly with computed tomography infarct volume at 5-7 days, mRS and BI at 3 and 12 months. Neopterin was raised in patients at 5-7 d, relative to controls, and in subjects with significant atherosclerosis. Spontaneous IL-1beta, TNF-alpha and IL-6 gene and protein expression by blood cells was minimal, and induction of these cytokines by lipopolysaccharide (LPS) was significantly lower in patients than in controls during the first week. Minimum LPS-induced cytokine production correlated strongly with mRS and BI, and also with plasma cortisol.
Absence of spontaneous whole blood gene activation or cytokine production suggests that peripheral blood cells are not the source of cytokines measured in plasma after AIS. Increased plasma IL-1ra within 12 h of AIS onset, the relationship between sTNF-RI and stroke severity, and suppressed cytokine induction suggests early activation of endogenous immunosuppressive mechanisms after AIS.
细胞因子作为局部和全身炎症反应的关键介质,在缺血性卒中后于脑内产生。在卒中患者的循环系统中已检测到一些细胞因子,但其作用和来源尚不清楚。主要聚焦于白细胞介素(IL)-1相关机制,我们对36例在急性缺血性卒中(AIS)后12小时内入组并随访1年的患者,连续测量了血浆炎症标志物以及全血中细胞因子的产生情况。
与年龄、性别和动脉粥样硬化匹配的对照组相比,入院时血浆IL-1受体拮抗剂(IL-1ra)浓度升高。IL-1β、可溶性II型IL-1受体、肿瘤坏死因子(TNF)-α、TNF-RII、IL-10和瘦素浓度与对照组无显著差异,但第一周的可溶性I型TNF受体(sTNF-RI)峰值与5-7天时的计算机断层扫描梗死体积、3个月和12个月时的改良Rankin量表(mRS)评分及巴氏指数(BI)密切相关。与对照组相比,患者在5-7天时新蝶呤升高,在有显著动脉粥样硬化的受试者中也是如此。血细胞自发产生的IL-1β、TNF-α和IL-6基因及蛋白表达极少,在第一周内,患者经脂多糖(LPS)诱导产生的这些细胞因子明显低于对照组。LPS诱导的细胞因子产生最低值与mRS评分和BI密切相关,也与血浆皮质醇相关。
全血无自发基因激活或细胞因子产生表明,外周血细胞不是AIS后血浆中所测细胞因子的来源。AIS发病12小时内血浆IL-1ra升高、sTNF-RI与卒中严重程度的关系以及细胞因子诱导受抑制表明,AIS后内源性免疫抑制机制早期激活。
