Eid Raymond E, Rao Deepak A, Zhou Jing, Lo Sheng-fu L, Ranjbaran Hooman, Gallo Amy, Sokol Seth I, Pfau Steven, Pober Jordan S, Tellides George
Interdepartmental Program in Vascular Biology and Therapeutics and Department of Surgery, Yale University School of Medicine, New Haven, Conn., USA.
Circulation. 2009 Mar 17;119(10):1424-32. doi: 10.1161/CIRCULATIONAHA.108.827618. Epub 2009 Mar 2.
Atherosclerosis is an inflammatory disease in which interferon (IFN)-gamma, the signature cytokine of Th1 cells, plays a central role. We investigated whether interleukin (IL)-17, the signature cytokine of Th17 cells, is also associated with human coronary atherosclerosis.
Circulating IL-17 and IFN-gamma were detected in a subset of patients with coronary atherosclerosis and in referent outpatients of similar age without cardiac disease but not in young healthy individuals. IL-17 plasma levels correlated closely with those of the IL-12/IFN-gamma/CXCL10 cytokine axis but not with known Th17 inducers such as IL-1beta, IL-6, and IL-23. Both IL-17 and IFN-gamma were produced at higher levels by T cells within cultured atherosclerotic coronary arteries after polyclonal activation than within nondiseased vessels. Combinations of proinflammatory cytokines induced IFN-gamma but not IL-17 secretion. Blockade of IFN-gamma signaling increased IL-17 synthesis, whereas neutralization of IL-17 responses decreased IFN-gamma synthesis; production of both cytokines was inhibited by transforming growth factor-beta1. Approximately 10-fold fewer coronary artery-infiltrating T helper cells were IL-17 producers than IFN-gamma producers, and unexpectedly, IL-17/IFN-gamma double producers were readily detectable within the artery wall. Although IL-17 did not modulate the growth or survival of cultured vascular smooth muscle cells, IL-17 interacted cooperatively with IFN-gamma to enhance IL-6, CXCL8, and CXCL10 secretion.
Our findings demonstrate that IL-17 is produced concomitantly with IFN-gamma by coronary artery-infiltrating T cells and that these cytokines act synergistically to induce proinflammatory responses in vascular smooth muscle cells.
动脉粥样硬化是一种炎症性疾病,其中Th1细胞的标志性细胞因子γ干扰素发挥核心作用。我们研究了Th17细胞的标志性细胞因子白细胞介素(IL)-17是否也与人类冠状动脉粥样硬化相关。
在一部分冠状动脉粥样硬化患者以及年龄相仿但无心脏病的对照门诊患者中检测到循环中的IL-17和γ干扰素,而在年轻健康个体中未检测到。IL-17血浆水平与IL-12/γ干扰素/CXCL10细胞因子轴密切相关,但与已知的Th17诱导因子如IL-1β、IL-6和IL-23无关。多克隆激活后,培养的动脉粥样硬化冠状动脉内的T细胞产生的IL-17和γ干扰素水平均高于未患病血管内的T细胞。促炎细胞因子组合诱导γ干扰素分泌,但不诱导IL-17分泌。阻断γ干扰素信号传导可增加IL-17合成,而中和IL-17反应则降低γ干扰素合成;两种细胞因子的产生均受到转化生长因子-β1的抑制。冠状动脉浸润的辅助性T细胞中,产生IL-17的细胞比产生γ干扰素的细胞少约10倍,出乎意料的是,在动脉壁内很容易检测到IL-17/γ干扰素双产生细胞。虽然IL-17不调节培养的血管平滑肌细胞的生长或存活,但IL-17与γ干扰素协同作用可增强IL-6、CXCL8和CXCL10的分泌。
我们的研究结果表明,冠状动脉浸润的T细胞同时产生IL-17和γ干扰素,并且这些细胞因子协同作用,在血管平滑肌细胞中诱导促炎反应。
