首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Leukotriene E4: perspective on the forgotten mediator.
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Leukotriene E4: perspective on the forgotten mediator.

机译:白三烯E4:对被遗忘的介体的看法。

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摘要

Leukotriene (LT) E(4) mediates many of the principal features of bronchial asthma, such as bronchial constriction, hyperresponsiveness, eosinophilia, and increased vascular permeability. Furthermore, it is the most stable of the cysteinyl leukotrienes (CysLTs) and can be active at the site of release for a prolonged time after its synthesis. There might be several reasons why LTE(4) has been forgotten. LTE(4) demonstrated low affinity for CysLT(1) and CysLT(2) receptors in equilibrium competition assays. It was less potent than other CysLTs in functional assays, such as calcium flux, in cells transfected with CysLT(1) and CysLT(2). The introduction of CysLT(1) antagonists into clinical practice diverted interest into CysLT(1)-related mechanisms, which were mediated mainly by LTD(4). However, experiments with animal models and human studies have revealed that LTE(4) has unique characteristics that cannot be explained by the current knowledge of CysLT(1) and CysLT(2). These activities include its potencyrelative to other CysLTs to increase airway responsiveness to histamine, to enhance eosinophilic recruitment, and to increase vascular permeability. Asthmatic airways also demonstrate marked in vivo relative hyperresponsiveness to LTE(4), especially in patients with aspirin-sensitive respiratory disease. This has stimulated a search for additional LT receptors that would respond preferentially to LTE(4) stimulation.
机译:白三烯(LT)E(4)介导了支气管哮喘的许多主要特征,例如支气管收缩,反应过度,嗜酸性粒细胞增多和血管通透性增加。此外,它是半胱氨酰白三烯(CysLTs)中最稳定的,在合成后的较长时间内可在释放位点起作用。 LTE(4)被遗忘的原因可能有多种。 LTE(4)在平衡竞争测定中证明对CysLT(1)和CysLT(2)受体的亲和力低。在用CysLT(1)和CysLT(2)转染的细胞中,在功能测定(例如钙通量)中,它的效力不如其他CysLT。将CysLT(1)拮抗剂引入临床实践使人们对CysLT(1)相关的机制产生了兴趣,这些机制主要由LTD(4)介导。但是,通过动物模型和人体研究进行的实验表明,LTE(4)具有独特的特性,目前的CysLT(1)和CysLT(2)知识无法解释。这些活动包括其相对于其他CysLTs的效力,以增加对组胺的气道反应性,增强嗜酸性的募集并增加血管通透性。哮喘气道在体内对LTE(4)也表现出明显的相对高反应性,尤其是在阿司匹林敏感的呼吸系统疾病患者中。这刺激了对其他LT受体的搜索,这些受体将优先响应LTE(4)刺激。

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