Literature DB >> 10436082

The immunoglobulin fold family: sequence analysis and 3D structure comparisons.

D M Halaby1, A Poupon, J Mornon.   

Abstract

Fifty-two 3D structures of Ig-like domains covering the immunoglobulin fold family (IgFF) were compared and classified according to the conservation of their secondary structures. Members of the IgFF are distantly related proteins or evolutionarily unrelated proteins with a similar fold, the Ig fold. In this paper, a multiple structural alignment of the conserved common core is described and the correlation between corresponding sequences is discussed. While the members of the IgFF exhibit wide heterogeneity in terms of tissue and species distribution or functional implications, the 3D structures of these domains are far more conserved than their sequences. We define topologically equivalent residues in the Ig-like domains, describe the hydrophobic common cores and discuss the presence of additional strands. The disulfide bridges, not necessary for the stability of the Ig fold, may have an effect on the compactness of the domains. Based upon sequence and structure analysis, we propose the introduction of two new subtypes (C3 and C4) to the previous classifications, in addition to a new global structural classification. The very low mean sequence identity between subgroups of the IgFF suggests the occurrence of both divergent and convergent evolutionary processes, explaining the wide diversity of the superfamily. Finally, this review suggest that hydrophobic residues constituting the common hydrophobic cores are important clues to explain how highly divergent sequences can adopt a similar fold.

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Year:  1999        PMID: 10436082     DOI: 10.1093/protein/12.7.563

Source DB:  PubMed          Journal:  Protein Eng        ISSN: 0269-2139


  90 in total

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Journal:  J Bacteriol       Date:  2005-02       Impact factor: 3.490

6.  Energetics of aliphatic deletions in protein cores.

Authors:  Marta Bueno; Luis A Campos; Jorge Estrada; Javier Sancho
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7.  Consequences of domain insertion on sequence-structure divergence in a superfold.

Authors:  Chetanya Pandya; Shoshana Brown; Ursula Pieper; Andrej Sali; Debra Dunaway-Mariano; Patricia C Babbitt; Yu Xia; Karen N Allen
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8.  Hepatitis C virus E2 envelope glycoprotein core structure.

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9.  The UL6 gene product forms the portal for entry of DNA into the herpes simplex virus capsid.

Authors:  W W Newcomb; R M Juhas; D R Thomsen; F L Homa; A D Burch; S K Weller; J C Brown
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10.  Structure and dynamics of Ca2+-binding domain 1 of the Na+/Ca2+ exchanger in the presence and in the absence of Ca2+.

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Journal:  J Mol Biol       Date:  2008-01-30       Impact factor: 5.469

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