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疟疾病媒按蚊的抗血小板蛋白具有体内抗血栓作用,而不会影响止血功能。

Anopheline anti-platelet protein from a malaria vector mosquito has anti-thrombotic effects in vivo without compromising hemostasis.

机构信息

First Institute of New Drug Discovery, Otsuka Pharmaceutical Company Limited, Tokushima, Japan.

出版信息

Thromb Res. 2012 Feb;129(2):169-75. doi: 10.1016/j.thromres.2011.09.015. Epub 2011 Oct 9.

Abstract

INTRODUCTION

The saliva of blood-feeding animals (e.g., mosquitoes, ticks, bats) has pharmacological activities that facilitate efficient blood-sucking. We previously identified a unique anti-platelet protein, anopheline anti-platelet protein (AAPP), from the salivary gland of female Anopheles stephensi (human malaria vector mosquito). AAPP specifically blocks platelet adhesion to collagen by binding directly to collagen and subsequently aggregating platelets. To examine the potential of AAPP as a therapeutic agent, we investigated the in vivo anti-thrombotic effects of AAPP.

MATERIALS AND METHODS

Effects of AAPP on whole blood/platelet aggregation in mice were examined. AAPP was also challenged in an established model of pulmonary thromboembolism in mice. We simultaneously investigated the side-effects of the protein (prolongation of bleeding time and coagulation time). Aspirin was used as a positive control for comparison of anti-thrombotic effects.

RESULTS AND CONCLUSIONS

AAPP inhibited whole blood aggregation induced by collagen at 10mg/kg body weight. AAPP prevented pulmonary death at a lower dose (3mg/kg) without prolongation of bleeding time compared with aspirin (100mg/kg) that compromised hemostasis. AAPP and aspirin did not affect coagulation time. These results indicate that AAPP has great potential as a new anti-platelet agent with a better risk/benefit ratio than that seen with aspirin (the most widely used anti-platelet agent).

摘要

简介

吸血动物(例如蚊子、蜱虫、蝙蝠)的唾液具有促进高效吸血的药理学活性。我们之前从雌性按蚊(人类疟疾传播媒介蚊子)的唾液腺中鉴定出一种独特的抗血小板蛋白,即疟原虫抗血小板蛋白(AAPP)。AAPP 通过直接结合胶原蛋白并随后聚集血小板,特异性地阻止血小板与胶原蛋白的黏附。为了研究 AAPP 作为治疗剂的潜力,我们研究了 AAPP 的体内抗血栓形成作用。

材料和方法

在小鼠中检查 AAPP 对全血/血小板聚集的影响。还在小鼠肺血栓栓塞模型中对 AAPP 进行了挑战。我们同时研究了该蛋白的副作用(出血时间和凝血时间延长)。阿司匹林被用作抗血栓形成效果比较的阳性对照。

结果与结论

AAPP 在 10mg/kg 体重时抑制了由胶原蛋白诱导的全血聚集。与阿司匹林(100mg/kg)相比,AAPP 在不延长出血时间的情况下,以较低剂量(3mg/kg)预防了肺死亡,而阿司匹林会损害止血功能。AAPP 和阿司匹林均不影响凝血时间。这些结果表明,AAPP 具有作为新型抗血小板药物的巨大潜力,其风险/收益比优于阿司匹林(最广泛使用的抗血小板药物)。

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