Thematic Review Series: Fat-Soluble Vitamins: Vitamin K: Recent trends in the metabolism and cell biology of vitamin K with special reference to vitamin K cycling and MK-4 biosynthesis |
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Authors: | Martin J. Shearer Paul Newman |
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Affiliation: | *Centre for Haemostasis and Thrombosis, Guy''s and St. Thomas’ NHS Foundation Trust, London SE1 7EH, UK; and;†Cancer Research UK London Research Institute, London WC2A 3LY, UK |
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Abstract: | In contrast to other fat-soluble vitamins, dietary vitamin K is rapidly lost to the body resulting in comparatively low tissue stores. Deficiency is kept at bay by the ubiquity of vitamin K in the diet, synthesis by gut microflora in some species, and relatively low vitamin K cofactor requirements for γ-glutamyl carboxylation. However, as shown by fatal neonatal bleeding in mice that lack vitamin K epoxide reductase (VKOR), the low requirements are dependent on the ability of animals to regenerate vitamin K from its epoxide metabolite via the vitamin K cycle. The identification of the genes encoding VKOR and its paralog VKOR-like 1 (VKORL1) has accelerated understanding of the enzymology of this salvage pathway. In parallel, a novel human enzyme that participates in the cellular conversion of phylloquinone to menaquinone (MK)-4 was identified as UbiA prenyltransferase-containing domain 1 (UBIAD1). Recent studies suggest that side-chain cleavage of oral phylloquinone occurs in the intestine, and that menadione is a circulating precursor of tissue MK-4. The mechanisms and functions of vitamin K recycling and MK-4 synthesis have dominated advances made in vitamin K biochemistry over the last five years and, after a brief overview of general metabolism, are the main focuses of this review. |
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Keywords: | phylloquinone, menaquinones, vitamin K epoxide, γ -carboxyglutamate proteins, vitamin K antagonists, anticoagulants, warfarin, warfarin resistance, vitamin K epoxide reductase, vitamin K dehydrogenase, UbiA prenyltransferase-containing domain 1 |
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