β-环糊精十四硫酸盐，一种新型环状寡糖，可抑制冠状动脉血管损伤后的血栓形成和新生内膜形成。

Beta-cyclodextrin tetradecasulfate, a novel cyclic oligosaccharide, inhibits thrombus and neointimal formation after coronary vascular injury.

作者信息

Meneveau Nicolas F, Klugherz Bruce D, Chaqour Brahim, Anand Vibha, Tomaszewski John E, Joullié Madeleine M, Macarak Edward, Golden Michael, Weisz Paul B, Wilensky Robert L

机构信息

Department of Medicine, University of Pennsylvania, USA.

出版信息

Coron Artery Dis. 2002 May;13(3):189-97. doi: 10.1097/00019501-200205000-00009.

DOI:10.1097/00019501-200205000-00009

PMID:12131024

Abstract

BACKGROUND

Neointimal formation is a major cause of restenosis after interventional vascular procedures. Beta-cyclodextrin tetradecasulfate (beta-CDT) has been shown to inhibit fibroblast growth factor activity and we hypothesized that beta-CDT would reduce intimal formation.

DESIGN

Three studies were performed: (1) pharmacokinetics of oral and intravenous beta-CDT and determination of optimal dose, (2) determination of efficacy of oral and intravenous beta-CDT in reducing neointimal formation after balloon-overstretch injury and (3) determination of the effect of beta-CDT on cellular proliferation, factor Xa activity, activated clotting time, activated partial thromboplastin time and thrombus formation.

METHODS

Pharmacokinetics were determined in eight domestic swine following administration of oral beta-CDT and intravenous beta-CDT at three doses each. In the efficacy study, balloon-overstretch injury of 37 pigs (69 arteries) was performed and randomized into three groups (n = 23 arteries/group): control, oral administration of 300 mg beta-CDT/kg per day or intravenous infusion of 100 mg beta-CDT/kg per day. Animals were sacrificed 14 days later. Cellular proliferation and mural thrombus were determined in six arteries/group at 5 days and endothelial coverage was evaluated at 5 and 14 days.

RESULTS

Oral and intravenous beta-CDT reduced the intimal hyperplasia area normalized to injury index by 24 and 48%, respectively: control, 3.03 +/- 0.75 mm2, oral, 2.31 +/- 0.83 mm2 (P = 0.004) and intravenous, 1.67 +/- 0.73 mm2 (P = 0.0000002). beta-CDT reduced cellular proliferation (control, 55 +/- 18%, oral, 35 +/- 7%, P = 0.03 and intravenous, 30 +/- 12%, P = 0.01) and mural thrombus formation (control, 0.84 +/- 0.4 mm2, oral, 0.44 +/- 0.14 mm2, P = 0.04, intravenous, 0.42 +/- 0.09 mm2, P = 0.03). Endothelial coverage was increased in the experimental groups (P = 0.008, oral versus control, P < 0.0001, intravenous versus control). Factor Xa activity was inhibited 9-10 fold following intravenous administration while oral administration demonstrated no effect.

CONCLUSIONS

Both oral and intravenous formation of beta-CDT reduced intimal hyperplasia with the greatest reduction in the intravenous group. We postulate that beta-CDT was effective by the combination of increasing endothelial coverage, reducing mural thrombus formation, inhibiting factor Xa activity and reducing cellular proliferation.

摘要

背景

血管介入术后新生内膜形成是再狭窄的主要原因。β-环糊精十四硫酸钠（β-CDT）已被证明可抑制成纤维细胞生长因子活性，我们推测β-CDT可减少内膜形成。

设计

进行了三项研究：（1）口服和静脉注射β-CDT的药代动力学及最佳剂量的确定；（2）口服和静脉注射β-CDT在球囊过度扩张损伤后减少新生内膜形成的疗效确定；（3）β-CDT对细胞增殖、因子Xa活性、活化凝血时间、活化部分凝血活酶时间和血栓形成的影响确定。

方法

给八只家猪分别口服和静脉注射三种剂量的β-CDT，测定药代动力学。在疗效研究中，对37头猪（69条动脉）进行球囊过度扩张损伤，并随机分为三组（每组23条动脉）：对照组、每天口服300mgβ-CDT/kg或每天静脉输注100mgβ-CDT/kg。14天后处死动物。在第5天每组取6条动脉测定细胞增殖和壁血栓，在第5天和第14天评估内皮覆盖情况。

结果

口服和静脉注射β-CDT分别使内膜增生面积与损伤指数的比值降低了24%和48%：对照组为3.03±0.75mm²，口服组为2.31±0.83mm²（P = 0.004），静脉注射组为1.67±0.73mm²（P = 0.0000002）。β-CDT减少了细胞增殖（对照组为55±18%，口服组为35±7%，P = 0.03，静脉注射组为30±12%，P = 0.01）和壁血栓形成（对照组为0.84±0.4mm²，口服组为0.44±0.14mm²，P = 0.04，静脉注射组为0.42±0.09mm²，P = 0.03）。实验组的内皮覆盖增加（口服组与对照组比较，P = 0.008；静脉注射组与对照组比较，P < 0.0001）。静脉给药后因子Xa活性被抑制9 - 10倍，而口服给药无此作用。