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High-throughput methods for identification of protein-protein interactions involving short linear motifs

机译:鉴定涉及短线性基序的蛋白质相互作用的高通量方法

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Interactions between modular domains and short linear motifs (3–10 amino acids peptide stretches) are crucial for cell signaling. The motifs typically reside in the disordered regions of the proteome and the interactions are often transient, allowing for rapid changes in response to changing stimuli. The properties that make domain-motif interactions suitable for cell signaling also make them difficult to capture experimentally and they are therefore largely underrepresented in the known protein-protein interaction networks. Most of the knowledge on domain-motif interactions is derived from low-throughput studies, although there exist dedicated high-throughput methods for the identification of domain-motif interactions. The methods include arrays of peptides or proteins, display of peptides on phage or yeast, and yeast-two-hybrid experiments. We here provide a survey of scalable methods for domain-motif interaction profiling. These methods have frequently been applied to a limited number of ubiquitous domain families. It is now time to apply them to a broader set of peptide binding proteins, to provide a comprehensive picture of the linear motifs in the human proteome and to link them to their potential binding partners. Despite the plethora of methods, it is still a challenge for most approaches to identify interactions that rely on post-translational modification or context dependent or conditional interactions, suggesting directions for further method development.
机译:模块化结构域和短线性基序(3-10个氨基酸的肽段)之间的相互作用对于细胞信号传导至关重要。这些基序通常位于蛋白质组的无序区域,并且相互作用通常是瞬时的,从而允许响应于变化的刺激而快速变化。使域-基序相互作用适合细胞信号转导的特性也使它们难以通过实验捕获,因此在已知的蛋白质-蛋白质相互作用网络中,它们的代表性大大不足。尽管存在专用的高通量方法来识别域-基元相互作用,但有关域-基元相互作用的大多数知识都来自低通量研究。该方法包括肽或蛋白质的阵列,在噬菌体或酵母上展示肽以及酵母两杂交实验。我们在这里提供了域主题交互分析的可伸缩方法的概述。这些方法经常被应用于有限数量的普遍存在的域族。现在是时候将它们应用到更广泛的肽结合蛋白上,以提供人蛋白质组中线性基序的全面情况,并将它们与潜在的结合伴侣连接起来。尽管有很多方法,但是对于大多数依赖于翻译后修饰或依赖于上下文或条件的交互来识别交互的方法,仍然是一个挑战,为进一步开发方法提供了方向。

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