Ephrin B4型受体激活可在体外减少人隐静脉新生内膜增生。
Ephrin type-B receptor 4 activation reduces neointimal hyperplasia in human saphenous vein in vitro.
作者信息
Wong Daniel J, Lu Daniel Y, Protack Clinton D, Kuwahara Go, Bai Hualong, Sadaghianloo Nirvana, Tellides George, Dardik Alan
机构信息
Vascular Biology and Therapeutics (VBT) Program and the Department of Surgery, Yale University School of Medicine, New Haven, Conn.
Vascular Biology and Therapeutics (VBT) Program and the Department of Surgery, Yale University School of Medicine, New Haven, Conn; Department of Surgery, VA Connecticut Healthcare System, West Haven, Conn.
出版信息
J Vasc Surg. 2016 Mar;63(3):795-804. doi: 10.1016/j.jvs.2014.09.036. Epub 2014 Oct 24.
BACKGROUND
Vein bypass is an essential therapy for patients with advanced peripheral and coronary artery disease despite development of neointimal hyperplasia. We have shown that stimulation of the receptor tyrosine kinase ephrin type-B receptor 4 (Eph-B4) with its ligand ephrin-B2 prevents neointimal hyperplasia in murine vein grafts. This study determines whether Eph-B4 in adult human veins is capable of phosphorylation and activation of downstream signaling pathways, as well as functional to release nitric oxide (NO) and prevent neointimal hyperplasia in vitro.
METHODS
Discarded human saphenous veins were taken from the operating room and placed in organ culture without or with ephrin-B2/Fc (2 μg/mL) for 14 days, and the neointima/media ratio was measured in matched veins. Primary human umbilical vein endothelial cells were treated with ephrin-B2/Fc (2 μg/mL) and examined with quantitative polymerase chain reaction, Western blot, immunoassays, and for release of NO. Ephrin-B2/Fc (2 μg/mL) was placed on the adventitia of saphenous veins treated with arterial shear stress for 24 hours in a bioreactor and activated Eph-B4 examined with immunofluorescence.
RESULTS
The baseline intima/media ratio in saphenous vein rings was 0.456 ± 0.097, which increased to 0.726 ± 0.142 in untreated veins after 14 days in organ culture but only to 0.630 ± 0.132 in veins treated with ephrin-B2/Fc (n = 19, P = .017). Ephrin-B2/Fc stimulated Akt, endothelial NO synthase and caveolin-1 phosphorylation, and NO release (P = .007) from human umbilical vein endothelial cells (n = 6). Ephrin-B2/Fc delivered to the adventitia stimulated endothelial Eph-B4 phosphorylation after 24 hours of arterial stress in a bioreactor (n = 3).
CONCLUSIONS
Eph-B4 is present and functional in adult human saphenous veins, with intact downstream signaling pathways capable of NO release and prevention of neointimal hyperplasia in vitro. Adventitial delivery of ephrin-B2/Fc activates endothelial Eph-B4 in saphenous veins treated with arterial shear stress in vitro. These results suggest that stimulation of Eph-B4 function may be a candidate strategy for translation to human clinical trials designed to inhibit venous neointimal hyperplasia.
背景
尽管存在新生内膜增生,但静脉搭桥术仍是晚期外周动脉疾病和冠状动脉疾病患者的重要治疗方法。我们已经证明,用其配体ephrin-B2刺激受体酪氨酸激酶Ephrin B型受体4(Eph-B4)可预防小鼠静脉移植物中的新生内膜增生。本研究确定成人静脉中的Eph-B4是否能够磷酸化并激活下游信号通路,以及在体外是否具有释放一氧化氮(NO)和预防新生内膜增生的功能。
方法
从手术室获取废弃的人隐静脉,置于器官培养中,不添加或添加ephrin-B2/Fc(2μg/mL)培养14天,测量配对静脉的新生内膜/中膜比值。用人脐静脉内皮细胞用ephrin-B2/Fc(2μg/mL)处理,并用定量聚合酶链反应、蛋白质印迹、免疫测定法检测,并检测NO的释放。将ephrin-B2/Fc(2μg/mL)置于生物反应器中经动脉剪切应力处理24小时的隐静脉外膜上,用免疫荧光法检测活化的Eph-B4。
结果
隐静脉环的基线内膜/中膜比值为0.456±0.097,在器官培养14天后,未处理的静脉中该比值增加到0.726±0.142,但在ephrin-B2/Fc处理的静脉中仅增加到0.630±0.132(n = 19,P = 0.017)。Ephrin-B2/Fc刺激人脐静脉内皮细胞(n = 6)中的Akt、内皮型一氧化氮合酶和小窝蛋白-1磷酸化以及NO释放(P = 0.007)。在生物反应器中经动脉应激24小时后,递送至外膜的Ephrin-B2/Fc刺激内皮Eph-B4磷酸化(n = 3)。
结论
Eph-B4在成人隐静脉中存在且具有功能,其下游信号通路完整,能够在体外释放NO并预防新生内膜增生。在体外经动脉剪切应力处理的隐静脉中,外膜递送ephrin-B2/Fc可激活内皮Eph-B4。这些结果表明,刺激Eph-B4功能可能是转化为旨在抑制静脉新生内膜增生的人体临床试验的候选策略。
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