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Target Identification for Small Bioactive Molecules: Finding the Needle in the Haystack

机译:小型生物活性分子的目标识别:在干草堆中寻找针头

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摘要

Identification and confirmation of bioactive small-molecule targets is a crucial, often decisive step both in academic and pharmaceutical research. Through the development and availability of several new experimental techniques, target identification is, in principle, feasible, and the number of successful examples steadily grows. However, a generic methodology that can successfully be applied in the majority of the cases has not yet been established. Herein we summarize current methods for target identification of small molecules, primarily for a chemistry audience but also the biological community, for example, the chemist or biologist attempting to identify the target of a given bioactive compound. We describe the most frequently employed experimental approaches for target identification and provide several representative examples illustrating the state-of-the-art. Among the techniques currently available, protein affinity isolation using suitable small-molecule probes (pulldown) and subsequent mass spectrometric analysis of the isolated proteins appears to be most powerful and most frequently applied. To provide guidance for rapid entry into the field and based on our own experience we propose a typical workflow for target identification, which centers on the application of chemical proteomics as the key step to generate hypotheses for potential target proteins.
机译:在学术和药物研究中,鉴定和确认具有生物活性的小分子靶标都是至关重要的,通常是决定性的步骤。通过开发和提供几种新的实验技术,目标识别从原则上讲是可行的,成功实例的数量稳步增长。但是,尚未建立可以成功应用于大多数情况的通用方法。本文中,我们总结了目前用于小分子目标识别的方法,主要是针对化学读者,也包括生物界,例如,试图鉴定给定生物活性化合物目标的化学家或生物学家。我们描述了用于目标识别的最常用的实验方法,并提供了一些代表性的例子来说明最新技术。在当前可用的技术中,使用合适的小分子探针进行蛋白质亲和分离(下拉)以及随后对分离出的蛋白质进行质谱分析似乎是最有效和最常用的技术。为了为快速进入该领域提供指导,并根据我们自己的经验,我们提出了一种典型的靶标识别工作流程,该流程以化学蛋白质组学的应用为中心,这是生成潜在靶蛋白假设的关键步骤。

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