Literature DB >> 18156468

Identification of transient hub proteins and the possible structural basis for their multiple interactions.

Miho Higurashi1, Takashi Ishida, Kengo Kinoshita.   

Abstract

Proteins that can interact with multiple partners play central roles in the network of protein-protein interactions. They are called hub proteins, and recently it was suggested that an abundance of intrinsically disordered regions on their surfaces facilitates their binding to multiple partners. However, in those studies, the hub proteins were identified as proteins with multiple partners, regardless of whether the interactions were transient or permanent. As a result, a certain number of hub proteins are subunits of stable multi-subunit proteins, such as supramolecules. It is well known that stable complexes and transient complexes have different structural features, and thus the statistics based on the current definition of hub proteins will hide the true nature of hub proteins. Therefore, in this paper, we first describe a new approach to identify proteins with multiple partners dynamically, using the Protein Data Bank, and then we performed statistical analyses of the structural features of these proteins. We refer to the proteins as transient hub proteins or sociable proteins, to clarify the difference with hub proteins. As a result, we found that the main difference between sociable and nonsociable proteins is not the abundance of disordered regions, in contrast to the previous studies, but rather the structural flexibility of the entire protein. We also found greater predominance of charged and polar residues in sociable proteins than previously reported.

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Year:  2008        PMID: 18156468      PMCID: PMC2144588          DOI: 10.1110/ps.073196308

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  31 in total

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Review 6.  Intrinsically unstructured proteins: re-assessing the protein structure-function paradigm.

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  34 in total

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Review 2.  Sequence, structure, function, immunity: structural genomics of costimulation.

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5.  Integration of protein motions with molecular networks reveals different mechanisms for permanent and transient interactions.

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6.  Exploring functional roles of multibinding protein interfaces.

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7.  Computational analysis of C-reactive protein for assessment of molecular dynamics and interaction properties.

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Review 9.  Hub promiscuity in protein-protein interaction networks.

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