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(钆螯合物)-苯丙氨酸-组氨酸-半胱氨酸-脯氨酸(羟基)-酪氨酸(2-氯)-天冬氨酸-亮氨酸-半胱氨酸-组氨酸-异亮氨酸-亮氨酸-(钆螯合物)

(Gd-chelate)-Phe-His-Cys-Pro(OH)-Tyr(2-Cl)-Asp-Leu-Cys-His-Ile-Leu-(Gd-chelate)

作者信息

Zhang Huiming

机构信息

National Center for Biotechnology Information, NLM, NIH, Bethesda, MD,

Abstract

The acute formation of thrombus after atherosclerotic plaque rupture has been well recognized as the cause of unstable angina, myocardial infarction, transient ischemic attacks, and stroke (1, 2). Platelets and fibrin are the major components of all thrombi involved in the development and progression of atherosclerotic disease (3). MRI has shown promise in thrombus detection in both animals and humans (4), such as direct thrombus imaging based on the T-shortening properties of endogenous methemogobin in venous thrombi (5) and enhancing the contrast between the myocardium and intracardiac by conventional gadolinium chelates (6). However, thrombosis is a dynamic process in which the thrombus material of different ages forms a layered structure due to successive mural deposition (7). MR signal of thrombi is complicated by the presence of platelets, fibrin, and red blood cells in the clots (7). Accurate thrombus age definition and detection of old and organized thrombi remain difficult. Since fibrin is abundant in all types of thrombi, including arterial, venous, acute, and chronic, fibrin-targeted contrast agents can be used to differentiate between layers of fibrin deposits in all types of thrombi and in superimposed thrombosis associated with plaque (3). The low concentration of fibrin present in plasma minimizes spurious background imaging signal (3). Fibrin is formed after thrombin cleavage of fibrinopeptide A from fibrinogen Aα-chains, followed by polymerization and cross-linkage to form thick fibrin bundles and complex branched clot network (8). 4GdPeptide is a gadolinium based contrast agent designed to bind to fibrin (7). 4GdPeptide comprises a small peptide of 11 amino acids and two gadolinium chelates such as gadolinium-diethylenetriaminepentaacetic acid (Gd-DTPA) or gadolinium-1,4,7,10-tetraazcyclododecane--tetraacetate (Gd-DOTA) attached to each terminal (7, 9). Gd-DOTA has an stability five orders of magnitude greater than that of Gd-DTPA (10). This greater stability reduces the toxicity caused by the dissociation of free Gd(III) in the metabolic process (10). The small peptide contains one intramolecular disulfur bond, and binds to fibrin selectively and reversibly (9, 11). The binding to fibrin generates a field dependent paramagnetic enhancement effect (PRE) due to the increase of the effective rotation correlation time τ (12). No interactions and competitive binding with other proteins such as fibrinogen or collagen have been noted in both or (11). 4GdPeptide can penetrate through thrombi to bind fibrin in depth passive diffusion; and distinguish between occlusive and non-occlusive arterial thrombi or between thrombi of different sizes and ages (11). Early-phase clinical studies (phase I and II) are currently testing the safety of 4GdPeptide in humans (11).

摘要

动脉粥样硬化斑块破裂后血栓的急性形成已被公认为是不稳定型心绞痛、心肌梗死、短暂性脑缺血发作和中风的病因(1,2)。血小板和纤维蛋白是参与动脉粥样硬化疾病发生和发展的所有血栓的主要成分(3)。磁共振成像(MRI)在动物和人类血栓检测方面已显示出前景(4),例如基于静脉血栓中内源性高铁血红蛋白的T缩短特性进行直接血栓成像(5),以及通过传统的钆螯合物增强心肌与心腔内的对比度(6)。然而,血栓形成是一个动态过程,不同年龄的血栓物质由于连续的壁层沉积而形成分层结构(7)。血栓中的血小板、纤维蛋白和红细胞使血栓的磁共振信号变得复杂(7)。准确界定血栓年龄以及检测陈旧性和机化性血栓仍然困难。由于纤维蛋白在所有类型的血栓中都很丰富,包括动脉血栓、静脉血栓、急性血栓和慢性血栓,因此靶向纤维蛋白的造影剂可用于区分所有类型血栓中纤维蛋白沉积物的层以及与斑块相关的叠加血栓中的层(3)。血浆中纤维蛋白浓度较低,可将虚假的背景成像信号降至最低(3)。纤维蛋白是在凝血酶从纤维蛋白原Aα链上裂解掉纤维蛋白肽A后形成的,随后聚合并交联形成粗大的纤维蛋白束和复杂的分支凝块网络(8)。4GdPeptide是一种设计用于与纤维蛋白结合的钆基造影剂(7)。4GdPeptide由一个11个氨基酸的小肽和两个钆螯合物组成,如钆 - 二乙烯三胺五乙酸(Gd - DTPA)或钆 - 1,4,7,10 - 四氮杂环十二烷 - 四乙酸(Gd - DOTA),分别连接在每个末端(7,9)。Gd - DOTA的稳定性比Gd - DTPA高五个数量级(10)。这种更高的稳定性降低了代谢过程中游离Gd(III)解离所导致的毒性(10)。小肽含有一个分子内二硫键,能选择性且可逆地与纤维蛋白结合(9,11)。与纤维蛋白的结合由于有效旋转相关时间τ的增加而产生场依赖性顺磁增强效应(PRE)(12)。在体内或体外均未观察到与其他蛋白质如纤维蛋白原或胶原蛋白的相互作用和竞争性结合(11)。4GdPeptide可通过被动扩散穿透血栓以深入结合纤维蛋白;并区分闭塞性和非闭塞性动脉血栓或不同大小和年龄的血栓(11)。早期临床研究(I期和II期)目前正在测试4GdPeptide在人体中的安全性(11)。

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