Literature DB >> 20696150

Molecular and biochemical characterization of human galactokinase and its small molecule inhibitors.

M Tang1, K Wierenga, L J Elsas, K Lai.   

Abstract

Human galactokinase (GALK) is the first enzyme in the Leloir pathway, converting α-d-galactose into galactose-1-phosphate (Gal-1-P). Recently, there is increasing interest in targeting GALK as a novel therapy to ameliorate the disease manifestations in patients with Classic Galactosemia as it would, in combination with (ga-)lactose restriction reduce accumulation of Gal-1-P, a cytotoxic agent. Previously, we identified 34 small molecule compounds that inhibited GALK in vitro using experimental high-throughput screening. In order to isolate useful lead compounds, we characterized these hits with regards to their kinase selectivity profiles, potency and capability to reduce Gal-1-P accumulation in patient cell lines, and their modes of action. We found that the majority of these compounds had IC(50)s ranging from 0.7μM to 33.3μM. When tested against other members of the GHMP kinase family, three compounds (1, 4, and 24) selectively inhibited GALK with high potency. Through alignment of GALK and mevalonate kinase (MVK) crystal structures, we identified that eight amino acid residues and an L1 loop were different within the ATP-binding pockets of these two closely related kinases. By site-directed mutagenesis experiments, we identified one amino acid residue required for the inhibitory function of two of the three selective compounds. Based on these results, we generated binding models of these two compounds using a high-precision docking program. Compounds 4 and 24 inhibited GALK in a mixed model, while compound 1 exhibited parabolic competitive inhibition. Most importantly, using cells from galactosemic patients we found that selected compounds lowered Gal-1-P concentrations.
Copyright © 2010 Elsevier Ireland Ltd. All rights reserved.

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Year:  2010        PMID: 20696150      PMCID: PMC2980576          DOI: 10.1016/j.cbi.2010.07.025

Source DB:  PubMed          Journal:  Chem Biol Interact        ISSN: 0009-2797            Impact factor:   5.192


  32 in total

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4.  Glide: a new approach for rapid, accurate docking and scoring. 1. Method and assessment of docking accuracy.

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Journal:  J Med Chem       Date:  2004-03-25       Impact factor: 7.446

5.  Galactose metabolism in a patient with hereditary galactokinase deficiency.

Authors:  R Gitzelmann; H J Wells; S Segal
Journal:  Eur J Clin Invest       Date:  1974-04       Impact factor: 4.686

6.  Regulation of genes controlling synthesis of the galactose pathway enzymes in yeast.

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7.  Galactitol and galactose-1-phosphate in the lens of a galactosemic infant.

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  13 in total

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Review 4.  Innovative therapy for Classic Galactosemia - tale of two HTS.

Authors:  M Tang; S I Odejinmi; H Vankayalapati; K J Wierenga; K Lai
Journal:  Mol Genet Metab       Date:  2011-10-01       Impact factor: 4.797

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Authors:  M Tang; S I Odejinmi; Y M Allette; H Vankayalapati; K Lai
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Review 6.  Medical management of chronic liver diseases in children (part I): focus on curable or potentially curable diseases.

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Review 7.  Is prenatal myo-inositol deficiency a mechanism of CNS injury in galactosemia?

Authors:  Gerard T Berry
Journal:  J Inherit Metab Dis       Date:  2011-01-19       Impact factor: 4.982

8.  pH-rate profiles support a general base mechanism for galactokinase (Lactococcus lactis).

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Review 10.  Sweet and sour: an update on classic galactosemia.

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