4.6 Article

Large-scale phosphomimetic screening identifies phospho-modulated motif-based protein interactions

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MOLECULAR SYSTEMS BIOLOGY
卷 -, 期 -, 页码 -

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WILEY
DOI: 10.15252/msb.202211164

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clathrin; phage display; phosphomimetic mutation; phosphorylation; protein-protein interactions

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Phosphorylation is a common post-translation modification that regulates protein function through protein-protein interactions. We created a phosphomimetic peptide-phage display library to discover phosphosites that modulate short linear motif-based interactions. Our research identified 248 phosphosites that modulate motif-mediated interactions, and we studied the phospho-dependent interaction between clathrin and HURP in detail. The structural characterization of the clathrin-HURP complex revealed the molecular basis for the phospho-dependency. Our work demonstrates the importance of phosphomimetic ProP-PD in discovering novel phospho-modulated interactions essential for cellular function.
Phosphorylation is a ubiquitous post-translation modification that regulates protein function by promoting, inhibiting or modulating protein-protein interactions. Hundreds of thousands of phosphosites have been identified but the vast majority have not been functionally characterised and it remains a challenge to decipher phosphorylation events modulating interactions. We generated a phosphomimetic proteomic peptide-phage display library to screen for phosphosites that modulate short linear motif-based interactions. The peptidome covers similar to 13,500 phospho-serine/threonine sites found in the intrinsically disordered regions of the human proteome. Each phosphosite is represented as wild-type and phosphomimetic variant. We screened 71 protein domains to identify 248 phosphosites that modulate motif-mediated interactions. Affinity measurements confirmed the phospho-modulation of 14 out of 18 tested interactions. We performed a detailed follow-up on a phospho-dependent interaction between clathrin and the mitotic spindle protein hepatoma-upregulated protein (HURP), demonstrating the essentiality of the phospho-dependency to the mitotic function of HURP. Structural characterisation of the clathrin-HURP complex elucidated the molecular basis for the phospho-dependency. Our work showcases the power of phosphomimetic ProP-PD to discover novel phospho-modulated interactions required for cellular function.

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