Characterization of vitamin K–dependent carboxylase mutations that cause bleeding and nonbleeding disorders

Tie, Jian Ke; Carneiro, Jorge David Aivazoglou; Jin, Da Yun; Martinhago, Ciro Dresh; Vermeer, Cees; Stafford, Darrel W.

doi:10.1182/blood-2015-10-677633

Cited by 43 publications

(68 citation statements)

References 49 publications

(58 reference statements)

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“…The cDNA of GGCX or its mutants was cloned into mammalian expression vector pBudCE4.1-Met.Luc and transiently expressed in the GGCX-deficient dual-reporter cells as described in Section 3.3. Four hours posttransfection, the transfection medium was replaced by complete growth medium containing 11 μ M vitamin K and incubated for 48 h. Carboxylation activity was determined by measuring the level of carboxylated reporter proteins in the cell culture medium using sandwich-based ELISA (Tie et al, 2016). …”

Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

“…Using this cell-based assay, we first studied GGCX mutations found in a child with severe cerebral bleeding and comorbid Keutel syndrome, a nonbleeding malady caused by functional defects of MGP (Tie et al, 2016). Clinical data showed that high doses of vitamin K administration improved the bleeding diathesis of the patient, but not the functional defect of MGP.…”

Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

“…Menaquinone supplementation has been shown to improve extrahepatic vitamin K status, but to have no effect on thrombin generation in healthy subjects (Theuwissen et al, 2012). However, results from the GGCX-deficient cell-based assay show that both vitamin K and menaquinones can efficiently support the carboxylation of both coagulation factors and MGP by wild-type GGCX (Tie et al, 2016). The different contributions of phylloquinone and menaquinones to hepatic and extrahepatic carboxylation may therefore be caused by the way different tissue absorbs and utilizes these K vitamins.…”

Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

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Functional Study of the Vitamin K Cycle Enzymes in Live Cells

Tie

Stafford

2017

Methods in Enzymology

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Vitamin K-dependent carboxylation, an essential posttranslational modification catalyzed by gamma-glutamyl carboxylase, is required for the biological functions of proteins that control blood coagulation, vascular calcification, bone metabolism, and other important physiological processes. Concomitant with carboxylation, reduced vitamin K (KH2) is oxidized to vitamin K epoxide (KO). KO must be recycled back to KH2 by the enzymes vitamin K epoxide reductase and vitamin K reductase in a pathway known as the vitamin K cycle. Our current knowledge about the enzymes of the vitamin K cycle is mainly based on in vitro studies of each individual enzymes under artificial conditions, which are of limited usefulness in understanding how the complex carboxylation process is carried out in the physiological environment. In this chapter, we review the current in vitro activity assays for vitamin K cycle enzymes. We describe the rationale, establishment, and application of cell-based assays for the functional study of these enzymes in the native cellular milieu. In these cell-based assays, different vitamin K-dependent proteins were designed and stably expressed in mammalian cells as reporter proteins to accommodate the readily used enzyme-linked immunosorbent assay for carboxylation efficiency evaluation. Additionally, recently emerged genome-editing techniques TALENs and CRISPR-Cas9 were used to knock out the endogenous enzymes in the reporter cell lines to eliminate the background. These cell-based assays are easy to scale up for high-throughput screening of inhibitors of vitamin K cycle enzymes and have been successfully used to clarify the genotypes and their clinical phenotypes of enzymes of the vitamin K cycle.

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Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

Section: Functional Study Of Ggcx Using Crispr-cas9-mediated Gene mentioning

confidence: 99%

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Functional Study of the Vitamin K Cycle Enzymes in Live Cells

Tie

Stafford

2017

Methods in Enzymology

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“…It is also possible that this splice-site mutation could result in several variant mRNA transcripts of GGCX, as has previously described for other genes (Gallinaro et al , 2006; Kallabi et al , 2015). The affected patients reported by Kariminejad et al (2014) have normal coagulation factor carboxylation, but defects in their MGP carboxylation; it is therefore possible that some of the mRNA transcript may produce a GGCX mutant protein that causes MGP-carboxylation defects but has a smaller effect on coagulation factor carboxylation, as we have previously observed in a VKCFD patient (Tie et al , 2016). …”

Section: To the Editormentioning

confidence: 73%

“…This approach, unlike the traditional in vitro GGCX activity assay, allows us to assess the functionality of GGCX using its natural protein substrates in a cellular milieu that requires the enzyme to interact with its physiologic components for VKD carboxylation (Tie et al , 2016). Our result shows that the GGCX-Δex3 mutant abolished carboxylation activity for both reporter proteins (Figure 1a).…”

Section: To the Editormentioning

confidence: 99%

Splice-Site Mutation of Exon 3 Deletion in the Gamma-Glutamyl Carboxylase Gene Causes Inactivation of the Enzyme

Jin

Vermeer

Stafford

et al. 2016

Journal of Investigative Dermatology

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GGCX‐related congenital combined vitamin K‐dependent clotting factors deficiency‐1: Description of a fetus with chondrodysplasia punctata

Mathonnet

Cunat

Allias

et al. 2021

American J of Med Genetics Pt A

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Congenital combined vitamin K‐dependent clotting factors deficiency (VKCFD) is a rare autosomal recessive disease resulting in hemorrhagic symptoms usually associated with developmental disorders and bone abnormalities. Pathogenic variants in two genes encoding enzymes of the vitamin K cycle, GGCX and VKORC1, can lead to this disorder. We present the case of a male fetus with a brachytelephalangic chondrodysplasia punctata (CDP), absence of nasal bone, growth restriction, and bilateral ventriculomegaly at 18 weeks of gestation. Pathological examination showed a Binder phenotype, hypoplastic distal phalanges, stippled epiphyses, and brain abnormalities suggestive of a brain hemorrhage. Two GGCX pathogenic variants inherited respectively from the mother and the father were identified. To our knowledge, this is the first prenatal description of VKCFD. Even if it remains a rare etiology, which is mostly described in children or adult patients, VKCFD should be considered in fetuses with CDP.

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Characterization of vitamin K–dependent carboxylase mutations that cause bleeding and nonbleeding disorders

Cited by 43 publications

References 49 publications

Functional Study of the Vitamin K Cycle Enzymes in Live Cells

Functional Study of the Vitamin K Cycle Enzymes in Live Cells

Splice-Site Mutation of Exon 3 Deletion in the Gamma-Glutamyl Carboxylase Gene Causes Inactivation of the Enzyme

GGCX‐related congenital combined vitamin K‐dependent clotting factors deficiency‐1: Description of a fetus with chondrodysplasia punctata

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