Vitamin K antagonism aggravates chronic kidney disease-induced neointimal hyperplasia and calcification in arterialized veins: role of vitamin K treatment?

Emma Zaragatski; Jochen Grommes; Leon J. Schurgers; Stephan Langer; Lieven Kennes; Miriam Tamm; Thomas A. Koeppel; Jennifer Kranz; Tina Hackhofer; Karen Arakelyan; Michael J. Jacobs; Maria Kokozidou

doi:10.1038/ki.2015.298

Vitamin K antagonism aggravates chronic kidney disease-induced neointimal hyperplasia and calcification in arterialized veins: role of vitamin K treatment?

Emma Zaragatski, Jochen Grommes, Leon J. Schurgers, Stephan Langer, Lieven Kennes, Miriam Tamm, Thomas A. Koeppel, Jennifer Kranz, Tina Hackhofer, Karen Arakelyan, Michael J. Jacobs, Maria Kokozidou^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Arteriovenous fistula (AVF) is the common vascular access type for a hemodialysis patient. Its failure is due to neointimal hyperplasia. Vitamin K antagonists are given to lower thrombosis tendency, but have side effects that enhance arterial calcifications. Here, we investigated the effects of vitamin K antagonists and vitamin K2 (K2) treatment on neointimal hyperplasia development and calcification in rats and in arterialized human veins. AVF was generated in female rats while chronic kidney disease (CKD) was induced using an adenine-enriched diet. Arterialization, CKD, and vitamin K antagonists all significantly enhanced venous neointimal hyperplasia. K2 treatment, additional to vitamin K antagonists, significantly reduced neointimal hyperplasia in arterialized veins in healthy rats but not in rats with CKD. Arterialization, CKD, and vitamin K antagonism all significantly increased, whereas K2 supplementation attenuated calcification in healthy rats and rats with CKD. K2 significantly enhanced matrix Gla protein carboxylation in control rats and rats with CKD. Arterialized human vein samples contained inactive matrix Gla protein at calcification and neointimal hyperplasia sites, indicating local vitamin K deficiency. Thus, vitamin K antagonists have detrimental effects on AVF remodeling, whereas K2 reduced neointimal hyperplasia and calcification indicating vasoprotective effects. Hence, K2 administration may be useful to prevent neointimal hyperplasia and calcification in arterialized veins.

Original language	English
Pages (from-to)	601-611
Journal	Kidney International
Volume	89
Issue number	3
DOIs	https://doi.org/10.1038/ki.2015.298
Publication status	Published - Mar 2016

Keywords

cardiovascular disease
chronic kidney disease
hemodialysis
vascular calcification
uremia

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10.1038/ki.2015.298Licence: Free access - publisher

Cite this

Zaragatski, E., Grommes, J., Schurgers, L. J., Langer, S., Kennes, L., Tamm, M., Koeppel, T. A., Kranz, J., Hackhofer, T., Arakelyan, K., Jacobs, M. J., & Kokozidou, M. (2016). Vitamin K antagonism aggravates chronic kidney disease-induced neointimal hyperplasia and calcification in arterialized veins: role of vitamin K treatment? Kidney International, 89(3), 601-611. https://doi.org/10.1038/ki.2015.298

@article{d065caa8e9094bb5a4a63724409c9cf3,

title = "Vitamin K antagonism aggravates chronic kidney disease-induced neointimal hyperplasia and calcification in arterialized veins: role of vitamin K treatment?",

abstract = "Arteriovenous fistula (AVF) is the common vascular access type for a hemodialysis patient. Its failure is due to neointimal hyperplasia. Vitamin K antagonists are given to lower thrombosis tendency, but have side effects that enhance arterial calcifications. Here, we investigated the effects of vitamin K antagonists and vitamin K2 (K2) treatment on neointimal hyperplasia development and calcification in rats and in arterialized human veins. AVF was generated in female rats while chronic kidney disease (CKD) was induced using an adenine-enriched diet. Arterialization, CKD, and vitamin K antagonists all significantly enhanced venous neointimal hyperplasia. K2 treatment, additional to vitamin K antagonists, significantly reduced neointimal hyperplasia in arterialized veins in healthy rats but not in rats with CKD. Arterialization, CKD, and vitamin K antagonism all significantly increased, whereas K2 supplementation attenuated calcification in healthy rats and rats with CKD. K2 significantly enhanced matrix Gla protein carboxylation in control rats and rats with CKD. Arterialized human vein samples contained inactive matrix Gla protein at calcification and neointimal hyperplasia sites, indicating local vitamin K deficiency. Thus, vitamin K antagonists have detrimental effects on AVF remodeling, whereas K2 reduced neointimal hyperplasia and calcification indicating vasoprotective effects. Hence, K2 administration may be useful to prevent neointimal hyperplasia and calcification in arterialized veins. ",

keywords = "cardiovascular disease, chronic kidney disease, hemodialysis, vascular calcification, uremia",

author = "Emma Zaragatski and Jochen Grommes and Schurgers, {Leon J.} and Stephan Langer and Lieven Kennes and Miriam Tamm and Koeppel, {Thomas A.} and Jennifer Kranz and Tina Hackhofer and Karen Arakelyan and Jacobs, {Michael J.} and Maria Kokozidou",

year = "2016",

month = mar,

doi = "10.1038/ki.2015.298",

language = "English",

volume = "89",

pages = "601--611",

journal = "Kidney International",

issn = "0085-2538",

publisher = "Elsevier Science",