Vitamin K has important biological actions, mediated by the activation of vitamin K-dependent proteins (VKDPs), such as blood coagulation factors and other proteins involved in bone metabolism and in the inhibition of vascular calcifications. Table 1 summarizes the physiological function of the main VKDPs and the consequences of vitamin K deficiency in patients with chronic kidney disease (CKD) and normal renal function.

Vitamin K deficiency may result in the following: (a) anticoagulation with warfarin, a well-known inhibitor of vitamin K 2,3-epoxide reductase, vitamin K recycling (VKOR), an enzyme that recycles oxidized vitamin K to its reduced form; (b) inadequate dietary intake of vitamin K.

There are 2 main forms of vitamin K: K1 or phylloquinone, found in green vegetables, and K2 or menaquinones (MK-n), found in specific food (such as natto, in Japan) or derived from the metabolic activity of intestinal bacteria. MK-4 is the unique menaquinone produced by systemic conversion of phylloquinone to vitamin K2 through the action of prenyltransferase domain-containing protein 1 (UBIAD1) [1].

In this issue of the AJN, McCabe et al. [2] highlight, in a rat model of adenine-induced renal failure, how CKD can negatively affect vitamin K metabolism, generating a decreased expression of VKOR and utilization (γ-glutamyl carboxylase, Ggcx) enzymes in thoracic aorta. In addition, the uremic status was associated with a decrease in the kidney level of the phylloquinone to MK-4 bioconversion enzyme, UBIAD1. Thus, this study adds an important piece of understanding to the framework of the deranged vitamin K metabolism in CKD.

A reduced GGCX activity in the kidneys and in the aorta (but not in the liver) of uremic animals was previously found by Kaesler et al. [3], indicating that uremia per se affects the vitamin K system. In addition, supplementation of phylloquinone or menaquinone (MK-4) at pharmacological doses restored the abnormal vitamin K cycle activity and slowed the progression of vascular calcification [3].

Additional evidence is now available from studies in humans. An observational, prospective study of 167 CKD patients (stages 3-5) highlighted that patients with the CG/GG genotype of vitamin K epoxide reductase complex subunit 1 (the enzyme target of warfarin) had a higher risk of coronary artery calcification progression and poorer survival [4]. Taken together, these findings are consistent with the higher prevalence of vascular calcifications in hemodialysis patients, as well as with the observation of warfarin-associated increased calcifications in patients with CKD [5].

A reduced dietary intake may be an important additional cause of vitamin K deficiency in CKD patients, as indicated by previous studies, in part due to the dietary limitations imposed by the uremic status. Recently, we confirmed a low vitamin K1 intake in hemodialysis patients on a Mediterranean diet, compared to control subjects with normal renal function [6]. Participants completed a food journal of 7 consecutive days for the estimation of dietary intakes of macro- and micronutrients (minerals and vitamins). When considering the adequate vitamin K1 intake recommended in the literature, it was noted that there was a remarkable prevalence of reduced intake, which was approximately 70-90% less than normal. We found an average total daily vitamin K1 intake of 72 μg/day compared to 129 μg/day in healthy controls. However, when normalized per 1,000 kcal energy intake, dietary vitamin K1 was 47 μg in dialysis patients compared to 89 μg in controls [6]. Thus, CKD patients appear to be exposed to the negative effects of vitamin K deficiency for at least 2 reasons, that is, a reduced dietary intake and a reduced expression and activity of the VKOR enzymes. In addition, an increased prevalence of atrial fibrillation often requires starting warfarin treatment, with further inhibition of both hepatic and extra-hepatic VKDPs activity.

Therefore, assessing the vitamin K status could be potentially important in CKD patients, especially if studies on vitamin K supplementation will prove a positive effect on bone and vascular disorders [7]. Up to now, vitamin K administration to hemodialysis patients at pharmacological doses was tested with surrogate biomarkers indicating the vitamin K status, such as dephosphorylated undercarboxylated matrix Gla protein. Such studies highlighted an improvement of VKDPs function, proportional to the increase in dose [8,9]. More relevant outcomes such as bone disease, including fractures, vascular calcifications, cardiovascular morbidity and mortality are warranted. Indeed, studies evaluating the progression of vascular calcifications with vitamin K at pharmacological doses are currently in progress in CKD patients. The VitaVasK study in Europe ( identifier: NCT01742273) investigates the effects of phylloquinone (5 mg thrice weekly for 18 months) on the progression of thoracic aortic and coronary artery calcification. In Canada, the placebo-controlled iPACK HD study ( identifier: NCT01528800) also evaluates the progression of coronary artery calcifications but with a higher dose of phylloquinone and a shorter follow-up, 10 mg thrice weekly for 12 months.

In the process of establishing a physiopathological role of deranged vitamin K metabolism in CKD patients and the possibility of treatment of such abnormalities with an adequate cost-benefit ratio, several pieces of the puzzle are already in place. The experimental evidence provided by McCabe et al. [2] is a further step in the direction of establishing the uremic status as an independent risk factor of vitamin K deficiency and the deranged vitamin K metabolism in CKD as a therapeutic target.

Future studies should be implemented, addressing several undefined areas. First, more information is needed on the assessment of vitamin K status, possibly distinguishing phylloquinone and menaquinones, through standardized methods measuring undercarboxylated VKDPs and/or serum vitamin K levels. An effort should be made in determining the utility of vitamin K determination at the research and clinical level. Second, better characterization of vitamin K2 content in food is required, as the current available information is mainly related to vitamin K1. Dietary sources of vitamin K should be known both to the public and healthcare personnel. Third, more randomized placebo-controlled studies in CKD patients using phylloquinone, menaquinones or a combination of different vitamers should address the safety of vitamin K administration at high doses and relevant clinical outcomes, such as vascular calcifications, bone fractures, cardiovascular morbidity and mortality. Such studies should also assess the doses of vitamin K with the better cost- and risk-benefit ratio.

The authors have no conflict of interest to report.

Hirota Y, Nakagawa K, Sawada N, et al: Functional characterization of the vitamin K2 biosynthetic enzyme UBIAD1. PLoS One 2015;10:e0125737.
McCabe KM, Booth SL, Fu X, Ward E, Adams MA, Holden RM: Vitamin K metabolism in a rat model of chronic kidney disease. Am J Nephrol 2016;45:4-13.
Kaesler N, Magdeleyns E, Herfs M, et al: Impaired vitamin K recycling in uremia is rescued by vitamin K supplementation. Kidney Int 2014;86:286-293.
Holden RM, Booth SL, Tuttle A, et al: Sequence variation in vitamin K epoxide reductase gene is associated with survival and progressive coronary calcification in chronic kidney disease. Arterioscler Thromb Vasc Biol 2014;34:1591-1596.
Fusaro M, Tripepi G, Noale M, et al: Prevalence of vertebral fractures, vascular calcifications, and mortality in warfarin treated hemodialysis patients. Curr Vasc Pharmacol 2015;13:248-258.
Fusaro M, D'Alessandro C, Noale M, et al: Low vitamin K1 intake in haemodialysis patients. Clin Nutr 2016;pii:S0261-5614(16)30070-X.
Gallieni M, Fusaro M: Vitamin K and cardiovascular calcification in CKD: is patient supplementation on the horizon? Kidney Int 2014;86:232-234.
Caluwé R, Vandecasteele S, Van Vlem B, Vermeer C, De Vriese AS: Vitamin K2 supplementation in haemodialysis patients: a randomized dose-finding study. Nephrol Dial Transplant 2014;29:1385-1390.
Westenfeld R, Krueger T, Schlieper G, et al: Effect of vitamin K2 supplementation on functional vitamin K deficiency in hemodialysis patients: a randomized trial. Am J Kidney Dis 2012;59:186-195.
Copyright / Drug Dosage / Disclaimer
Copyright: All rights reserved. No part of this publication may be translated into other languages, reproduced or utilized in any form or by any means, electronic or mechanical, including photocopying, recording, microcopying, or by any information storage and retrieval system, without permission in writing from the publisher.
Drug Dosage: The authors and the publisher have exerted every effort to ensure that drug selection and dosage set forth in this text are in accord with current recommendations and practice at the time of publication. However, in view of ongoing research, changes in government regulations, and the constant flow of information relating to drug therapy and drug reactions, the reader is urged to check the package insert for each drug for any changes in indications and dosage and for added warnings and precautions. This is particularly important when the recommended agent is a new and/or infrequently employed drug.
Disclaimer: The statements, opinions and data contained in this publication are solely those of the individual authors and contributors and not of the publishers and the editor(s). The appearance of advertisements or/and product references in the publication is not a warranty, endorsement, or approval of the products or services advertised or of their effectiveness, quality or safety. The publisher and the editor(s) disclaim responsibility for any injury to persons or property resulting from any ideas, methods, instructions or products referred to in the content or advertisements.