Yen Ting-Lin, Wu Ming-Ping, Chung Chi-Li, Yang Wen-Bin, Jayakumar Thanasekaran, Geraldine Pitchairaj, Chou Chih-Ming, Chang Chia-Yau, Lu Wan-Jung, Sheu Joen-Rong
Graduate Institute of Medical Sciences and Department of Pharmacology, College of Medicine, Taipei Medical University, 250 Wu-Hsing St., Taipei, 110, Taiwan.
Department of Obstetrics and Gynecology, Chi-Mei Medical Center, Tainan, Taiwan.
J Biomed Sci. 2016 Feb 17;23:26. doi: 10.1186/s12929-016-0245-4.
Thrombus formation, a phenomenon primarily related to increased platelet activation, plays a key role in cardiovascular and cerebrovascular diseases. Although the established antiplatelet agents, such as aspirin and clopidogrel, have been shown to be beneficial in treating thromboembolic diseases, they have considerable limitations. Hence, the development of more effective and safe antithrombotic agents is necessary to satisfy a substantial unmet clinical need. In recent years, the favorable properties of imidazole-related drugs have prompted medicinal chemists to synthesize numerous novel therapeutic agents. The chemical structure of the benzimidazole backbone has proven antiplatelet properties. Moreover, synthetic oligosaccharides have exhibited antiplatelet properties. Therefore, we developed a new aldo-benzimidazole-derived oligosaccharide compound, M3BIM, for achieving a stronger antiplatelet effect than the drugs which are being used in clinical aspects. We investigated the effects of M3BIM on platelet activation ex vivo and its antithrombotic activity in vivo.
M3BIM (10-50 μM) exhibited a more potent activity in inhibiting platelet aggregation stimulated by collagen than it did in inhibiting that stimulated by thrombin in washed human platelets. The M3BIM treatment revealed no cytotoxicity in zebrafish embryos, even at the highest concentration of 100 μM. In addition, M3BIM inhibited the phosphorylation of phospholipase Cγ2, protein kinase C (PKC), and mitogen-activated protein kinases (MAPKs; extracellular signal-regulated kinase 2 and c-Jun N-terminal kinase 1), and markedly reduced the ATP-release reaction and intracellular calcium mobilization in collagen-activated platelets. By contrast, M3BIM showed no effects on either collagen-induced p38 MAPK and Akt phosphorylation or phorbol 12, 13-dibutyrate-induced PKC activation and platelet aggregation. Moreover, the M3BIM treatment substantially prolonged the closure time in human whole blood, and increased the occlusion time in mesenteric microvessels and attenuated cerebral infarction in mice. For the study of anticoagulant activities, M3BIM showed no significant effects in the prolongation of activated partial thromboplastin time and prothrombin time in mice.
The findings of our study suggest that M3BIM is a potential therapeutic agent for preventing or treating thromboembolic disorders.
血栓形成主要与血小板活化增加有关,在心血管和脑血管疾病中起关键作用。尽管已有的抗血小板药物,如阿司匹林和氯吡格雷,已被证明对治疗血栓栓塞性疾病有益,但它们有相当大的局限性。因此,开发更有效和安全的抗血栓药物对于满足大量未满足的临床需求是必要的。近年来,咪唑类药物的良好特性促使药物化学家合成了许多新型治疗剂。苯并咪唑骨架的化学结构已被证明具有抗血小板特性。此外,合成寡糖也表现出抗血小板特性。因此,我们开发了一种新的醛基苯并咪唑衍生的寡糖化合物M3BIM,以实现比临床使用的药物更强的抗血小板作用。我们研究了M3BIM对体外血小板活化的影响及其体内抗血栓活性。
在洗涤过的人血小板中,M3BIM(10 - 50 μM)在抑制胶原蛋白刺激的血小板聚集方面比抑制凝血酶刺激的血小板聚集表现出更强的活性。M3BIM处理在斑马鱼胚胎中未显示出细胞毒性,即使在最高浓度100 μM时也是如此。此外,M3BIM抑制磷脂酶Cγ2、蛋白激酶C(PKC)和丝裂原活化蛋白激酶(MAPKs;细胞外信号调节激酶2和c-Jun氨基末端激酶1)的磷酸化,并显著降低胶原蛋白激活的血小板中的ATP释放反应和细胞内钙动员。相比之下,M3BIM对胶原蛋白诱导的p38 MAPK和Akt磷酸化或佛波醇12,13 - 二丁酸诱导的PKC活化和血小板聚集均无影响。此外,M3BIM处理显著延长了人全血的凝血时间,并增加了肠系膜微血管的闭塞时间,减轻了小鼠的脑梗死。对于抗凝活性研究,M3BIM在延长小鼠活化部分凝血活酶时间和凝血酶原时间方面未显示出显著影响。
我们的研究结果表明,M3BIM是预防或治疗血栓栓塞性疾病的潜在治疗剂。
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