Literature DB >> 15096641

The NMR solution structure of the 30S ribosomal protein S27e encoded in gene RS27_ARCFU of Archaeoglobus fulgidis reveals a novel protein fold.

Catherine Herve du Penhoat1, Hanudatta S Atreya, Yang Shen, Gaohua Liu, Thomas B Acton, Rong Xiao, Zhaohui Li, Diana Murray, Gaetano T Montelione, Thomas Szyperski.   

Abstract

The Archaeoglobus fulgidis gene RS27_ARCFU encodes the 30S ribosomal protein S27e. Here, we present the high-quality NMR solution structure of this archaeal protein, which comprises a C4 zinc finger motif of the CX(2)CX(14-16)CX(2)C class. S27e was selected as a target of the Northeast Structural Genomics Consortium (target ID: GR2), and its three-dimensional structure is the first representative of a family of more than 116 homologous proteins occurring in eukaryotic and archaeal cells. As a salient feature of its molecular architecture, S27e exhibits a beta-sandwich consisting of two three-stranded sheets with topology B(decreasing), A(increasing), F(decreasing), and C(increasing), D(decreasing), E(increasing). Due to the uniqueness of the arrangement of the strands, the resulting fold was found to be novel. Residues that are highly conserved among the S27 proteins allowed identification of a structural motif of putative functional importance; a conserved hydrophobic patch may well play a pivotal role for functioning of S27 proteins, be it in archaeal or eukaryotic cells. The structure of human S27, which possesses a 26-residue amino-terminal extension when compared with the archaeal S27e, was modeled on the basis of two structural templates, S27e for the carboxy-terminal core and the amino-terminal segment of the archaeal ribosomal protein L37Ae for the extension. Remarkably, the electrostatic surface properties of archaeal and human proteins are predicted to be entirely different, pointing at either functional variations among archaeal and eukaryotic S27 proteins, or, assuming that the function remained invariant, to a concerted evolutionary change of the surface potential of proteins interacting with S27.

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Year:  2004        PMID: 15096641      PMCID: PMC2286747          DOI: 10.1110/ps.03589204

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


  47 in total

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  5 in total

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2.  The solution structure of ribosomal protein S17E from Methanobacterium thermoautotrophicum: a structural homolog of the FF domain.

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3.  Comparison of different torsion angle approaches for NMR structure determination.

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Journal:  Nucleic Acids Res       Date:  2007-08-01       Impact factor: 16.971

5.  Accurate de novo design of hyperstable constrained peptides.

Authors:  Gaurav Bhardwaj; Vikram Khipple Mulligan; Christopher D Bahl; Jason M Gilmore; Peta J Harvey; Olivier Cheneval; Garry W Buchko; Surya V S R K Pulavarti; Quentin Kaas; Alexander Eletsky; Po-Ssu Huang; William A Johnsen; Per Jr Greisen; Gabriel J Rocklin; Yifan Song; Thomas W Linsky; Andrew Watkins; Stephen A Rettie; Xianzhong Xu; Lauren P Carter; Richard Bonneau; James M Olson; Evangelos Coutsias; Colin E Correnti; Thomas Szyperski; David J Craik; David Baker
Journal:  Nature       Date:  2016-09-14       Impact factor: 49.962

  5 in total

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