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. 2018 May 24;399(6):565-576.
doi: 10.1515/hsz-2018-0109.

The two major glucokinase isoforms show conserved functionality in β-cells despite different subcellular distribution

Brian Lu  1   2 Miguel Munoz-Gomez  1 Yasuhiro Ikeda  1   2
Affiliations

The two major glucokinase isoforms show conserved functionality in β-cells despite different subcellular distribution

Brian Lu et al. Biol Chem. .

Abstract

Glucokinase (GCK) is crucial to regulating glucose metabolism in the liver and in pancreatic β-cells. There are two major GCK isoforms, hepatic and pancreatic GCKs, which differ only in exon 1. However, the functional differences between the two GCK isoforms remain poorly understood. Here, we used a β-cell-targeted gene transfer vector to determine the impact of isoform-specific GCK overexpression on β-cells in vitro and in vivo. We showed that pancreatic GCK had a nuclear localization signal unique to the pancreatic isoform, facilitating its nuclear distribution in β-cells. Despite the difference in subcellular distribution, overexpression of GCK isoforms similarly enhanced glucose uptake and β-cell proliferation in vitro. Overexpression of hepatic or pancreatic GCK also similarly enhanced β-cell proliferation in normal diet mice without affecting fasting glucose and intraperitoneal glucose tolerance tests (IPGTT). Our further study on human GCK sequences identified disproportional GCK amino acid variants in exon 1, while mutations linked to maturity onset diabetes of the young type 2 (MODY2) were disproportionally found in exons 2 through 10. Our results therefore indicate functional conservation between the two major GCK isoforms despite their distinct subcellular distribution.

Keywords: glucokinase; isoform; β-cell.

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References

    1. Ashkenazy, H., Abadi, S., Martz, E., Chay, O., Mayrose, I., Pupko, T., and Ben-Tal, N. (2016). ConSurf 2016: an improved methodology to estimate and visualize evolutionary conservation in macromolecules. Nucleic Acids Res. 44, W344–W350.
    1. Aukrust, I., Bjørkhaug, L., Negahdar, M., Molnes, J., Johansson, B.B., Müller, Y., Haas, W., Gygi, S.P., Søvik, O., Flatmark, T., et al. (2013). SUMOylation of pancreatic glucokinase regulates its cellular stability and activity. J. Biol. Chem. 288, 5951–5962.
    1. Baltrusch, S. and Tiedge, M. (2006). Glucokinase regulatory network in pancreatic β-cells and liver. Diabetes 55, S55–S64.
    1. Baltrusch, S., Lenzen, S., Okar, D.A., Lange, A.J., and Tiedge, M. (2001). Characterization of glucokinase-binding protein epitopes by a phage-displayed peptide library: identification of 6-phosphofructo-2-kinase/fructose-2,6-bisphosphatase as a novel interaction partner. J. Biol. Chem. 276, 43915–43923.
    1. Beck, T. and Miller, B.G. (2013). Structural basis for regulation of human glucokinase by glucokinase regulatory protein. Biochemistry 52, 6232–6239.

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