Extracellular matrix mineralization is regulated locally; different roles of two gla-containing proteins

Murshed, Monzur; Schinke, Thorsten; McKee, Marc D.; Karsenty, Gérard

doi:10.1083/jcb.200402046

Cited by 442 publications

(370 citation statements)

References 29 publications

(37 reference statements)

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“…Indication that such transformations could take place in the aortic wall has been provided by Watson et al (11) who showed that a subpopulation of cultured VSMCs were transformed to calcifying vascular cells (CVCs) capable of forming a mineralized matrix. We have shown (12) that BMP-2 and MGP are both synthesized by VSMCs and Murshed et al (13) have shown that MGP synthesized in the vessel wall and not blood born MGP is the in vivo pool of the protein that is active as the vascular calcification inhibitor. These findings emphasize the importance to understand the MGP-BMP-2 interaction in inhibition of vascular calcification.…”

mentioning

confidence: 74%

Effects of the blood coagulation vitamin K as an inhibitor of arterial calcification

Wallin

Schurgers

Wajih

2008

Thrombosis Research

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Introduction-The transformation of smooth muscle cells (VSMCs) in the vessel wall to osteoblast like cells is known to precede arterial calcification which may cause bleeding complications. The vitamin K-dependent protein MGP has been identified as an inhibitor of this process by binding BMP-2, a growth factor known to trigger the transformation. In this study, we determined if the vitamin K-dependent Gla region in MGP by itself can inhibit the growth factor activity of BMP-2 and if menaquinone-4 (MK4) regulates gene expression in VSMCs.

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mentioning

confidence: 74%

Effects of the blood coagulation vitamin K as an inhibitor of arterial calcification

Wallin

Schurgers

Wajih

2008

Thrombosis Research

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“…The ank/ank mice failed to thrive. 3,8,11,12 However, there was no significant difference in body weight of 10 male mice of each geno- Figure 7. Correction of increased calcification of ank/ank aortic ring explants and cultured SMCs by Vanin-1 gene knockout.…”

Section: Vanin-1 Knockout Does Not Suppress Calcification By Ank/ankmentioning

confidence: 99%

“…[1][2][3][4] Heritable deficiencies in mineralization regulators have been particularly informative about hierarchical, co-operative, and antagonistic relationships among such factors. 2,5,6 Indeed, the particularly potent capacity of PP i to inhibit hydroxyapatite crystal growth 7 has been underscored by the phenotypic effects of alteration of PP i transport and generation.…”

mentioning

confidence: 99%

Vanin-1 Pantetheinase Drives Increased Chondrogenic Potential of Mesenchymal Precursors in ank/ank Mice

Johnson

Yao

Lane

et al. 2008

The American Journal of Pathology

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Widespread endochondral and intramembranous ectopic bone formation is mediated by extracellular PP i deficiency that develops in ank/ank mice. Herein we report on the rapid condensation into chondrogenic nodules of cultured ank/ank bone marrow stromal cells (BMSCs). We compared the roles of increased chondrogenic potential versus altered osteoblast function in the ank/ank phenotype. To do so, we crossbred ank/ank mice with mice lacking Vanin-1 pantetheinase, which inhibits synthesis of the chondrogenesis regulator glutathione, since we observed increased Vanin-1 expression and pantetheinase activity and decreased glutathione in ank/ank BMSCs.

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“…In the vascular wall, the inhibition of γ-carboxylation of Glu residues yielded the undercarboxylation of MGP and the subsequent calcification of the tunica media [10]. Moreover, it has been shown in the bone tissue of transgenic mice, which produced two distinct mutated forms of MGP in osteoblasts, that the Gla residues are required for MGP antimineralization function [21].…”

Section: Discussionmentioning

confidence: 99%

Immunohistochemical localization and mRNA expression of matrix Gla protein and fetuin-A in bone biopsies of hemodialysis patients

et al. 2009

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Matrix Gla protein (MGP) and fetuin-A are inhibitors of arterial calcifications. In blood of rats, calcium-phosphate-fetuin-MGP complexes, produced in bone, have been identified. Indeed, an association between bone resorption, release of such complexes, and arterial calcifications has been reported. We have investigated the synthesis and localization of fetuin-A and MGP in bone of hemodialysis patients and the possible contribution of bone cells in arterial calcifications. Bone biopsies from 11 hemodialysis patients were used for histology, in situ hybridization of fetuin-A and MGP messenger RNA (mRNA), immunohistochemistry of fetuin-A, and total, carboxylated, and non-carboxylated MGP proteins. Patients showed various types of renal osteodystrophy, or normal bone. MGP was synthesized and expressed (total and carboxylated) by osteoblasts, osteocytes, and most osteoclasts, while fetuin-A by osteoblasts and osteocytes. Fetuin-A and carboxylated MGP proteins were positive in the calcified matrix, while total MGP was negative. Osteoid seams were negative to fetuin-A, lightly positive to carboxylated MGP, and occasionally positive to total MGP. Undercarboxylated MGP was mostly undetectable. In adult humans, fetuin-A is produced also by osteoblasts, and not only by hepatocytes, as previously believed. MGP, essentially carboxylated, is synthesized by osteoblasts and most osteoclasts. Increased bone turnover can be an important contributor to arterial calcifications.

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Extracellular matrix mineralization is regulated locally; different roles of two gla-containing proteins

Cited by 442 publications

References 29 publications

Effects of the blood coagulation vitamin K as an inhibitor of arterial calcification

Effects of the blood coagulation vitamin K as an inhibitor of arterial calcification

Vanin-1 Pantetheinase Drives Increased Chondrogenic Potential of Mesenchymal Precursors in ank/ank Mice

Immunohistochemical localization and mRNA expression of matrix Gla protein and fetuin-A in bone biopsies of hemodialysis patients

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