Inoue Teruo, Uchida Toshihiko, Yaguchi Isao, Sakai Yoshihiko, Takayanagi Kan, Morooka Shigenori
Department of Cardiology, Koshigaya Hospital, Dokkyo University School of Medicine, 2-1-50 Minamikoshigaya, Koshigaya City, Saitama 343-8555, Japan.
Circulation. 2003 Apr 8;107(13):1757-63. doi: 10.1161/01.CIR.0000060487.15126.56. Epub 2003 Mar 24.
Increased expression of the beta2 integrin Mac-1 (CD11b/CD18, alphaMbeta2), which is responsible for firm leukocyte adhesion to platelets and fibrinogen at injured vessels, is found in association with neointimal hyperplasia after coronary interventions. The role of Mac-1 in the pathophysiology of restenosis is incompletely defined. To clarify further the role of Mac-1, we determined whether coronary stenting induced activation of Mac-1, which is required for high-affinity receptor-ligand interactions.
Expression of CD11b (alpha-subunit of Mac-1) and binding of 8B2 (monoclonal antibody against an activation-dependent neoepitope of Mac-1) on the surface of polymorphonuclear leukocytes were analyzed in 62 patients undergoing coronary stenting using flow cytometric analysis of whole blood obtained from the coronary sinus and femoral vein. Transcardiac CD11b expression increased significantly at 24 hours and maximally at 48 hours after stenting; 8B2 began to increase at 10 minutes and was maximally increased at 48 hours after stenting. These changes were more prominent in patients with subsequent restenosis. Multiple regression analysis showed that the late lumen loss by quantitative coronary angiographic analysis was independently correlated with the CD11b increase (R=0.42, P<0.01) and the 8B2 increase (R=0.55, P<0.001) 48 hours after the procedure. Mac-1 activation, as assessed by 8B2 binding, was the most powerful predictor of late lumen loss.
Coronary stenting produced upregulation and early activation of the leukocyte integrin Mac-1, which is associated with late lumen loss and restenosis. These data support a role for inflammation in neointimal thickening and suggest the validity of targeting leukocyte recruitment for preventing clinical restenosis.
β2整合素Mac-1(CD11b/CD18,αMβ2)表达增加,其负责白细胞在损伤血管处与血小板和纤维蛋白原的牢固黏附,在冠状动脉介入治疗后与新生内膜增生相关。Mac-1在再狭窄病理生理学中的作用尚未完全明确。为进一步阐明Mac-1的作用,我们确定冠状动脉支架置入是否会诱导Mac-1的激活,而这是高亲和力受体-配体相互作用所必需的。
使用流式细胞术分析从冠状窦和股静脉采集的全血,对62例接受冠状动脉支架置入的患者多形核白细胞表面的CD11b(Mac-1的α亚基)表达及8B2(抗Mac-1激活依赖性新表位的单克隆抗体)结合情况进行分析。经心脏的CD11b表达在支架置入后24小时显著增加,48小时达到峰值;8B2在支架置入后10分钟开始增加,48小时达到最大增幅。这些变化在随后发生再狭窄的患者中更为显著。多元回归分析显示,定量冠状动脉造影分析得出的晚期管腔丢失与术后48小时CD11b增加(R = 0.42,P < 0.01)及8B2增加(R = 0.55,P < 0.001)独立相关。通过8B2结合评估的Mac-1激活是晚期管腔丢失最有力的预测指标。
冠状动脉支架置入导致白细胞整合素Mac-1上调和早期激活,这与晚期管腔丢失和再狭窄相关。这些数据支持炎症在新生内膜增厚中的作用,并提示靶向白细胞募集以预防临床再狭窄的有效性。
