Literature DB >> 29485124

Structure function relations in PDZ-domain-containing proteins: Implications for protein networks in cellular signalling.

G P Manjunath1, Praveena L Ramanujam, Sanjeev Galande.   

Abstract

Protein scaffolds as essential backbones for organization of supramolecular signalling complexes are a recurrent theme in several model systems. Scaffold proteins preferentially employ linear peptide binding motifs for recruiting their interaction partners. PDZ domains are one of the more commonly encountered peptide binding domains in several proteins including those involved in scaffolding functions. This domain is known for its promiscuity both in terms of ligand selection, mode of interaction with its ligands as well as its association with other protein interaction domains. PDZ domains are subject to several means of regulations by virtue of their functional diversity. Additionally, the PDZ domains are refractive to the effect of mutations and maintain their three-dimensional architecture under extreme mutational load. The biochemical and biophysical basis for this selectivity as well as promiscuity has been investigated and reviewed extensively. The present review focuses on the plasticity inherent in PDZ domains and its implications for modular organization as well as evolution of cellular signalling pathways in higher eukaryotes.

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Year:  2018        PMID: 29485124

Source DB:  PubMed          Journal:  J Biosci        ISSN: 0250-5991            Impact factor:   1.826


  173 in total

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7.  A multivalent PDZ-domain protein assembles signalling complexes in a G-protein-coupled cascade.

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9.  Hot spots for allosteric regulation on protein surfaces.

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  8 in total

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4.  PDZ Domains Across the Microbial World: Molecular Link to the Proteases, Stress Response, and Protein Synthesis.

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Review 7.  Specificity in PDZ-peptide interaction networks: Computational analysis and review.

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8.  A long isoform of GIV/Girdin contains a PDZ-binding module that regulates localization and G-protein binding.

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  8 in total

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