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发现哮喘药物的挑战日益增加。

The increasing challenge of discovering asthma drugs.

机构信息

Profectus Pharma Consulting Inc, San Jose, CA 95125, USA.

出版信息

Biochem Pharmacol. 2011 Sep 15;82(6):586-99. doi: 10.1016/j.bcp.2011.06.033. Epub 2011 Jul 2.

Abstract

The prevalence of asthma continues to rise. Current drugs provide symptomatic relief to some, but not all, patients. Despite the need for new therapeutics, and a huge research effort, only four novel agents from two classes of drugs - the antileukotrienes and an anti-IgE antibody - have been approved in the last 30 years. This review highlights three particular issues that contribute to the challenge of identifying new therapeutics. First is an over-reliance on animal models of allergy to define targets and expectations of efficacy that has met with poor translation to the clinical setting. While sensitivity to particular aeroallergens is one key risk factor for asthma, atopy and asthma are not synonymous, and while about half of adult asthmatics are atopic the incidence of allergic asthma is probably <50%. The second issue is a fundamental disconnect between the directions of basic research and clinical research. Basic research has developed a detailed, reductive, unifying mechanism of antigen-induced, T helper type 2 cell-mediated airway inflammation as the root cause of asthma. In contrast, clinical research has started to identify multiple asthma phenotypes with differing cellular components, mediators and sensitivities to asthma drugs, and probably varying underlying factors including susceptibility genes. Finally, different features of asthma - bronchoconstriction, symptoms, and exacerbations - respond diversely to treatment; effects that are not captured in animal models which do not develop asthma per se, but utilize unvalidated surrogate markers. Basic research needs to better integrate and utilize the clinical research findings to improve its relevance to drug discovery efforts.

摘要

哮喘的患病率持续上升。目前的药物为一些患者提供了症状缓解,但并非所有患者都有效。尽管需要新的治疗方法,并且进行了巨大的研究努力,但在过去的 30 年中,只有两种药物类别——抗白三烯和抗 IgE 抗体——批准了四种新型药物。这篇综述强调了导致鉴定新疗法具有挑战性的三个特殊问题。首先,过度依赖过敏的动物模型来定义靶点和疗效预期,导致这些靶点和预期在临床环境中的转化效果不佳。虽然对特定的气传过敏原的敏感性是哮喘的一个关键风险因素,但特应性和哮喘并非同义词,虽然约一半的成年哮喘患者是特应性的,但过敏性哮喘的发病率可能<50%。第二个问题是基础研究和临床研究之间的根本脱节。基础研究已经提出了一种详细、简化、统一的抗原诱导的 T 辅助 2 细胞介导的气道炎症机制,作为哮喘的根本原因。相比之下,临床研究已经开始确定具有不同细胞成分、介质和对哮喘药物敏感性的多种哮喘表型,并且可能具有不同的潜在因素,包括易感基因。最后,哮喘的不同特征——支气管收缩、症状和加重——对治疗的反应不同;这些特征在动物模型中无法捕捉到,因为动物模型本身不会发展成哮喘,而是利用未经验证的替代标志物。基础研究需要更好地整合和利用临床研究结果,以提高其对药物发现工作的相关性。

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