Vitamin K2 Regulation of Bone Homeostasis Is Mediated by the Steroid and Xenobiotic Receptor SXR

Tabb, Michelle M.; Sun, Aixu; Zhou, Changcheng; Grün, Felix; Errandi, Jody L.; Romero, Kimberly M.; Pham, Hang; Inoue, Satoshi; Mallick, Shyamali; Lin, Min; Forman, Barry M.; Blumberg, Bruce

doi:10.1074/jbc.m303136200

Cited by 338 publications

(279 citation statements)

References 71 publications

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“…Regulation of bone formation by vitamin K 2 may involve the γ-carboxylation of osteocalcin or may be mediated via the steroid and xenobiotic receptor (SXR) [13,27,[34][35][36]. However, it has also been reported that vitamin K 2 inhibits bone resorption via a mechanism that is independent of γ-carboxylation and related to its side chain [11].…”

Section: Introductionmentioning

confidence: 99%

Additive Effect of Vitamin K2 and Risedronate on Long Bone Mass in Hypophysectomized Young Rats

et al. 2007

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Section: Introductionmentioning

confidence: 99%

Additive Effect of Vitamin K2 and Risedronate on Long Bone Mass in Hypophysectomized Young Rats

et al. 2007

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“…The role of TERE1 in vitamin K-2, menaquinone, synthesis (Nakagawa et al, 2010) provides a highly probable and established mechanism of TERE1-mediated cholesterol modulation. Menaquinone is a known ligand for the nuclear receptor SXR (Tabb et al, 2003;Shearer and Newman, 2008;Zhou et al, 2009). SXR is known to heterodimerize with RXR and cross regulate LXR target genes that have wellestablished roles in modulation of cellular cholesterol efflux (Landes et al, 2003;Sonoda et al, 2005;Wang and Rader, 2007;Wang et al, , 2008bLim and Huang, 2008;Brown and Jessup, 2009;Zhou et al, 2009).…”

Section: Tere1 Modulation Of Cholesterolmentioning

confidence: 99%

The Bladder Tumor Suppressor Protein TERE1 (UBIAD1)Modulates Cell Cholesterol: Implications for Tumor Progression

Fredericks

McGarvey

Wang

et al. 2011

DNA and Cell Biology

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Convergent evidence implicates the TERE1 protein in human bladder tumor progression and lipid metabolism. Previously, reduced TERE1 expression was found in invasive urologic cancers and inhibited cell growth upon re-expression. A role in lipid metabolism was suggested by TERE1 binding to APOE, a cholesterol carrier, and to TBL2, a candidate protein in triglyceride disorders. Natural TERE1 mutations associate with Schnyder's corneal dystrophy, characterized by lipid accumulation. TERE1 catalyzes menaquinone synthesis, known to affect cholesterol homeostasis. To explore this relationship, we altered TERE1 and TBL2 dosage via ectopic expression and interfering RNA and measured cholesterol by Amplex red. Protein interactions of wild-type and mutant TERE1 with GST-APOE were evaluated by binding assays and molecular modeling. We conducted a bladder tumor microarray TERE1 expression analysis and assayed tumorigenicity of J82 cells ectopically expressing TERE1. TERE1 expression was reduced in a third of invasive specimens. Ectopic TERE1 expression in J82 bladder cancer cells dramatically inhibited nude mouse tumorigenesis. TERE1 and TBL2 proteins inversely modulated cellular cholesterol in HEK293 and bladder cancer cells from 20% to 50%. TERE1 point mutations affected APOE interactions, and resulted in cholesterol levels that differed from wild type. Elevated tumor cell cholesterol is known to affect apoptosis and growth signaling; thus, loss of TERE1 in invasive bladder cancer may represent a defect in menaquinone-mediated cholesterol homeostasis that contributes to progression.

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“…In feeding studies Spronk et al (16) showed that MK4 but not vitamin K 1 could prevent arterial calcification in rats when given in combination with warfarin. Certain combinations of vitamin K and warfarin given to rodents have been shown to inhibit vitamin K-dependent γ-carboxylation in extrahepatic tissues but not in the liver which maintains a normal coagulation system (18). As reduced vitamin K 1 and reduced MK4 are both cofactors in the γ-carboxylation system, this finding has raised questions about additional effects of MK4 in the arterial wall which may enhance inhibition of arterial calcification.…”

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confidence: 99%

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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Vitamin K2 Regulation of Bone Homeostasis Is Mediated by the Steroid and Xenobiotic Receptor SXR

Cited by 338 publications

References 71 publications

Additive Effect of Vitamin K2 and Risedronate on Long Bone Mass in Hypophysectomized Young Rats

Additive Effect of Vitamin K2 and Risedronate on Long Bone Mass in Hypophysectomized Young Rats

The Bladder Tumor Suppressor Protein TERE1 (UBIAD1)Modulates Cell Cholesterol: Implications for Tumor Progression

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

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