Literature DB >> 22694048

Stabilizing the heterologously expressed uric acid-xanthine transporter UapA from the lower eukaryote Aspergillus nidulans.

James Leung1, Alexander D Cameron, George Diallinas, Bernadette Byrne.   

Abstract

Despite detailed genetic and mutagenic analysis and a recent high-resolution structure of a bacterial member of the nucleobase-ascorbate transporter (NAT) family, understanding of the mechanism of action of eukaryotic NATs is limited. Preliminary studies successfully expressed and purified wild-type UapA to high homogeneity; however, the protein was extremely unstable, degrading almost completely after 48 h at 4°C. In an attempt to increase UapA stability we generated a number of single point mutants (E356D, E356Q, N409A, N409D, Q408E and G411V) previously shown to have reduced or no transport activity, but correct targeting to the membrane. The mutant UapA constructs expressed well as GFP fusions in Saccharomyces cerevisiae and exhibited similar fluorescent size exclusion chromatography (FSEC) profiles to the wild-type protein, following solubilization in 1% DDM, LDAO or OM + 1 mM xanthine. In order to assess the relative stabilities of the mutants, solubilized fractions prepared in 1% DDM + 1 mM xanthine were heated at 45°C for 10 min prior to FSEC. The Q408E and G411V mutants gave markedly better profiles than either wild-type or the other mutants. Further FSEC analysis following solubilization of the mutants in 1% NG ± xanthine confirmed that G411V is more stable than the other mutants, but showed that Q408E is unstable under these conditions. G411V and an N-terminally truncated construct G411VΔ1-11 were submitted to large-scale expression and purification. Long-term stability analysis revealed that G411VΔ1-11 was the most stable construct and the most suited to downstream structural studies.

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Year:  2012        PMID: 22694048     DOI: 10.3109/09687688.2012.690572

Source DB:  PubMed          Journal:  Mol Membr Biol        ISSN: 0968-7688            Impact factor:   2.857


  9 in total

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3.  Transfer of stabilising mutations between different secondary active transporter families.

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Journal:  FEBS Open Bio       Date:  2021-05-08       Impact factor: 2.792

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5.  Structure of eukaryotic purine/H(+) symporter UapA suggests a role for homodimerization in transport activity.

Authors:  Yilmaz Alguel; Sotiris Amillis; James Leung; George Lambrinidis; Stefano Capaldi; Nicola J Scull; Gregory Craven; So Iwata; Alan Armstrong; Emmanuel Mikros; George Diallinas; Alexander D Cameron; Bernadette Byrne
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6.  Tandem malonate-based glucosides (TMGs) for membrane protein structural studies.

Authors:  Hazrat Hussain; Jonas S Mortensen; Yang Du; Claudia Santillan; Orquidea Ribeiro; Juyeon Go; Parameswaran Hariharan; Claus J Loland; Lan Guan; Brian K Kobilka; Bernadette Byrne; Pil Seok Chae
Journal:  Sci Rep       Date:  2017-06-21       Impact factor: 4.379

7.  Structural Lipids Enable the Formation of Functional Oligomers of the Eukaryotic Purine Symporter UapA.

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8.  Identification of the substrate recognition and transport pathway in a eukaryotic member of the nucleobase-ascorbate transporter (NAT) family.

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Journal:  PLoS One       Date:  2012-07-25       Impact factor: 3.240

9.  Modelling and mutational analysis of Aspergillus nidulans UreA, a member of the subfamily of urea/H⁺ transporters in fungi and plants.

Authors:  Manuel Sanguinetti; Sotiris Amillis; Sergio Pantano; Claudio Scazzocchio; Ana Ramón
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  9 in total

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