Abstract
BackgroundWe examined the effects of the R325W mutation on the three-dimensional (3D) structure of the β-cell-specific Zn2+ (zinc) transporter ZnT-8.MethodsA model of the C-terminal domain of the human ZnT-8 protein was generated by homology modeling based on the known crystal structure of the Escherichia coli (E. coli) zinc transporter YiiP at 3.8 Å resolution.ResultsThe homodimer ZnT-8 protein structure exists as a Y-shaped architecture with Arg325 located at the ultimate bottom of this motif at approximately 13.5 Å from the transmembrane domain juncture. The C-terminal domain sequences of the human ZnT-8 protein and the E. coli zinc transporter YiiP share 12.3% identical and 39.5% homologous residues resulting in an overall homology of 51.8%. Validation statistics of the homology model showed a reasonable quality of the model. The C-terminal domain exhibited an αββαβ fold with Arg325 as the penultimate N-terminal residue of the α2-helix. The side chains of both Arg325 and Trp325 point away from the interface with the other monomer, whereas the ε-NH3+ group of Arg325 is predicted to form an ionic interaction with the β-COO- group of Asp326 as well as Asp295. An amino acid alignment of the β2-α2 C-terminal loop domain revealed a variety of neutral amino acids at position 325 of different ZnT-8 proteins.ConclusionsOur validated homology models predict that both Arg325 and Trp325, amino acids with a helix-forming behavior, and penultimate N-terminal residues in the α2-helix of the C-terminal domain, are shielded by the planar surface of the three cytoplasmic β-strands and hence unable to affect the sensing capacity of the C-terminal domain. Moreover, the amino acid residue at position 325 is too far removed from the docking and transporter parts of ZnT-8 to affect their local protein conformations. These data indicate that the inherited R325W abnormality in SLC30A8 may be tolerated and results in adequate zinc transfer to the correct sites in the pancreatic islet cells and are consistent with the observation that the SLC30A8 gene variant R325W has a low predicted value for future type 2 diabetes at population-based level.
Highlights
We examined the effects of the R325W mutation on the three-dimensional (3D) structure of the β-cellspecific Zn2+ transporter zinc transporter (ZnT)-8
Genome-wide association studies have currently identified single nucleotide polymorphisms (SNPs) within up to 10 genes associated with an increased risk of type 2 diabetes [2,3,4,5,6]
Structure quality factors - overall statistics sapiens ZnT-8 and E. coli zinc transporter YiiP sequences were aligned and with a typical homology modeling exercise, the most probable 3D models were created with the program Modeller, version 9 [27]
Summary
We examined the effects of the R325W mutation on the three-dimensional (3D) structure of the β-cellspecific Zn2+ (zinc) transporter ZnT-8. This report continues our analyses of the genetic factors playing an important role in the pathogenesis of type 2 diabetes [1]. Genome-wide association studies have currently identified single nucleotide polymorphisms (SNPs) within up to 10 genes associated with an increased risk of type 2 diabetes [2,3,4,5,6]. Several of the SNPs identified within or near these genes are hypothesized to influence β-cell function. Previous studies of the latter genes addi- Study. Total sample size; stage 1+2 (number of cases/controls) OR (95% CI) P-value Ref. DGI
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