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Review
. 2021 Apr:183:13-17.
doi: 10.1016/j.biochi.2020.11.001. Epub 2020 Nov 9.

The structural and molecular biology of type IV galactosemia

Affiliations
Review

The structural and molecular biology of type IV galactosemia

Samantha Banford et al. Biochimie. 2021 Apr.

Abstract

Type IV galactosemia is a recently discovered inherited metabolic disease. It is caused by mutations in the GALM gene which result in reduced activity of the enzyme galactose mutarotase. This enzyme catalyses the interconversion of the α- and β-anomers of d-galactose and some other monosaccharides. Human galactose mutarotase is monomeric and its structure is largely composed of β-sheets. The catalytic mechanism requires a histidine residue acting as an acid, and a glutamate acting as a base. Together, these residues open the pyranose ring of d-galactose enabling free rotation of the bond between the first two carbon atoms in the monosaccharide. This can cause reversal of the configuration of the hydroxyl group attached to carbon 1. Type IV galactosemia manifests with similar symptoms to type II galactosemia (galactokinase deficiency), i.e. early onset cataracts. However, as a recently discovered disease, the longer-term consequences are unknown. The physiological role, if any, of galactose mutarotase's reactions with other monosaccharides are not yet known. The possible associations with other proteins also require further investigation.

Keywords: Aldose 1-epimerase; Anomers; GALM; Galactose metabolism; Galactose mutarotase; Inherited metabolic disease.

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Conflict of interest statement

Declaration of competing interest None.

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