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心血管活性毒液毒素概述

Cardiovascular-Active Venom Toxins: An Overview.

作者信息

Rebello Horta Carolina Campolina, Chatzaki Maria, Rezende Bruno Almeida, Magalhães Bárbara de Freitas, Duarte Clara Guerra, Felicori Liza Figueiredo, Ribeiro Oliveira-Mendes Bárbara Bruna, do Carmo Anderson Oliveira, Chávez-Olórtegui Carlos, Kalapothakis Evanguedes

机构信息

Av. Antônio Carlos, 6627, Pampulha, Belo Horizonte, Minas Gerais, CEP 31270-901, Brazil.

出版信息

Curr Med Chem. 2016;23(6):603-22. doi: 10.2174/0929867323666160126142837.

Abstract

Animal venoms are a mixture of bioactive compounds produced as weapons and used primarily to immobilize and kill preys. As a result of the high potency and specificity for various physiological targets, many toxins from animal venoms have emerged as possible drugs for the medication of diverse disorders, including cardiovascular diseases. Captopril, which inhibits the angiotensin-converting enzyme (ACE), was the first successful venom-based drug and a notable example of rational drug design. Since captopril was developed, many studies have discovered novel bradykinin-potentiating peptides (BPPs) with actions on the cardiovascular system. Natriuretic peptides (NPs) have also been found in animal venoms and used as template to design new drugs with applications in cardiovascular diseases. Among the anti-arrhythmic peptides, GsMTx-4 was discovered to be a toxin that selectively inhibits the stretch-activated cation channels (SACs), which are involved in atrial fibrillation. The present review describes the main components isolated from animal venoms that act on the cardiovascular system and presents a brief summary of venomous animals and their venom apparatuses.

摘要

动物毒液是作为武器产生的生物活性化合物的混合物,主要用于使猎物失去活动能力并将其杀死。由于对各种生理靶点具有高效性和特异性,许多来自动物毒液的毒素已成为治疗包括心血管疾病在内的多种疾病的潜在药物。卡托普利是一种抑制血管紧张素转换酶(ACE)的药物,它是首个成功的基于毒液的药物,也是合理药物设计的一个显著例子。自卡托普利研发以来,许多研究发现了对心血管系统有作用的新型缓激肽增强肽(BPPs)。动物毒液中还发现了利钠肽(NPs),并将其用作设计治疗心血管疾病新药的模板。在抗心律失常肽中,GsMTx-4被发现是一种选择性抑制与心房颤动有关的牵张激活阳离子通道(SACs)的毒素。本综述描述了从动物毒液中分离出的作用于心血管系统的主要成分,并简要介绍了有毒动物及其毒液器官。

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