Allen S, Khan S, Tam S p, Koschinsky M, Taylor P, Yacoub M
Department of Cardiothoracic Surgery, Imperial College of Science, Technology and Medicine, Royal Brompton and Harefield NHS Trust Hospital, Harefield Hospital, Harefield, Middlesex UB9 6JH, United Kingdom.
FASEB J. 1998 Dec;12(15):1765-76. doi: 10.1096/fasebj.12.15.1765.
Lp(a) is a major inherited risk factor for premature atherosclerosis. The mechanism of Lp(a) atherogenicity has not been elucidated, but likely involves both its ability to interfere with plasminogen activation and its atherogenic potential as a lipoprotein particle after receptor-mediated uptake. We demonstrate that Lp(a) stimulates production of vascular cell adhesion molecule 1 (VCAM-1) and E-selectin in cultured human coronary artery endothelial cells (HCAEC). This effect resulted from a rise in intracellular free calcium induced by Lp(a) and could be inhibited by the intracellular calcium chelator, BAPTA/AM. The involvement of the LDL and VLDL receptors in Lp(a) activation of HCAEC were ruled out since Lp(a) induction of adhesion molecules was not prevented by an antibody (IgGC7) to the LDL receptor or by receptor-activating protein, an antagonist of ligand binding to the VLDL receptor. Addition of alpha2-macroglobulin as well as treatment with heparinase, chondroitinase ABC, and sodium chlorate did not decrease levels of VCAM-1 and E-selectin stimulated by Lp(a), suggesting that neither the low density lipoprotein receptor-related protein nor cell-surface proteoglycans are involved in Lp(a)-induced adhesion molecule production. Neither does the binding site on HCAEC responsible for adhesion molecule production by Lp(a) appear to involve plasminogen receptors, as levels of VCAM-1 and E-selectin were not significantly decreased by the addition of glu-plasminogen, the lysine analog epsilon-aminocaproic acid, or by trans-4-(aminomethyl)-cyclohexanecarboxymethylic acid (tranexamic acid), which acts by binding to the lysine binding sites carried on the kringle structures in plasminogen. In contrast, recombinant apolipoprotein (a) [r-apo(a)] competed with Lp(a) and attenuated the expression of VCAM-1 and E-selectin. In summary, we have identified a calcium-dependent interaction of Lp(a) with HCAEC capable of inducing potent surface expression of VCAM-1 and E-selectin that does not appear to involve any of the known potential Lp(a) binding sites. Because leukocyte recruitment to the vessel wall appears to represent one of the important early events in atherogenesis, this newly described endothelial cell-activating effect of Lp(a) places it at a crucial juncture in the initiation of atherogenic disease and may lead to a better understanding of the role of Lp(a) in the vascular biology of atherosclerosis.
脂蛋白(a)[Lp(a)]是早发性动脉粥样硬化的主要遗传风险因素。Lp(a)致动脉粥样硬化的机制尚未阐明,但可能涉及其干扰纤溶酶原激活的能力以及受体介导摄取后作为脂蛋白颗粒的致动脉粥样硬化潜力。我们证明,Lp(a)可刺激培养的人冠状动脉内皮细胞(HCAEC)中血管细胞黏附分子1(VCAM-1)和E选择素的产生。这种效应是由Lp(a)诱导的细胞内游离钙升高引起的,并且可以被细胞内钙螯合剂BAPTA/AM抑制。由于针对LDL受体的抗体(IgGC7)或受体激活蛋白(一种与VLDL受体配体结合的拮抗剂)不能阻止Lp(a)诱导黏附分子,因此排除了LDL和VLDL受体参与HCAEC的Lp(a)激活。添加α2巨球蛋白以及用肝素酶、软骨素酶ABC和氯酸钠处理均未降低Lp(a)刺激的VCAM-1和E选择素水平,这表明低密度脂蛋白受体相关蛋白和细胞表面蛋白聚糖均不参与Lp(a)诱导的黏附分子产生。HCAEC上负责Lp(a)产生黏附分子的结合位点似乎也不涉及纤溶酶原受体,因为添加谷氨酰胺纤溶酶原、赖氨酸类似物ε-氨基己酸或通过与纤溶酶原kringle结构上携带的赖氨酸结合位点结合而起作用的反式-4-(氨甲基)环己烷羧酸(氨甲环酸)均未显著降低VCAM-1和E选择素水平。相反,重组载脂蛋白(a)[r-apo(a)]与Lp(a)竞争并减弱了VCAM-1和E选择素的表达。总之,我们已经确定了Lp(a)与HCAEC之间的钙依赖性相互作用,这种相互作用能够诱导VCAM-1和E选择素在表面强力表达,而这似乎不涉及任何已知的潜在Lp(a)结合位点。由于白细胞募集到血管壁似乎是动脉粥样硬化发生过程中重要的早期事件之一,Lp(a)这种新描述的内皮细胞激活作用使其处于动脉粥样硬化疾病起始的关键节点,并且可能有助于更好地理解Lp(a)在动脉粥样硬化血管生物学中的作用。
