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Structural Evolution of the ABC Transporter Subfamily B

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Publication Date: 08 Nov 2007

Journal: Evolutionary Bioinformatics 2007:3 309-316

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Abstract Flanagan, J.U.1 and Huber, T.2

1ARC Special Research Centre for Functional and Applied Genomics, Level 5, Institute for Molecular Bioscience, The University of Queensland, St Lucia, QLD 4072, Australia. 2School of Molecular and Microbial Science, The University of Queensland, St Lucia, QLD 4072, Australia.

Abstract: The ATP binding cassette containing transporters are a superfamily of integral membrane proteins that translocate a wide range of substrates. The subfamily B members include the biologically important multidrug resistant (MDR) protein and the transporter associated with antigen processing (TAP) complex. Substrates translocated by this subfamily include drugs, lipids, peptides and iron. We have constructed a comprehensive set of comparative models for the transporters from eukaryotes and used these to study the effects of sequence divergence on the substrate translocation pathway. Notably, there is very little structural divergence between the bacterial template structure and the more distantly related eukaryotic proteins illustrating a need to conserve transporter structure. By contrast different properties have been adopted for the translocation pathway depending on the substrate type. A greater level of divergence in electrostatic properties is seen with transporters that have a broad substrate range both within and between species, while a high level of conservation is observed when the substrate range is narrow. This study represents the first effort towards understanding effect of evolution on subfamily B ABC transporters in the context of protein structure and biophysical properties.

Abbreviations: A. thaliana, Arabidopsis thaliana; D. melanogaster, Drosophilia melanogaster; S. aureus, Staphylococcus aureus; ABC, ATP binding cassette; TAP, Transporter associated with antigen processing.


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